← Back
Fetching drawings from USPTO…
Solid forms of 1-((S)-4-((R)-7-(6-amino-4-methyl-3-(trifluoromethyl)pyridin-2-yl)-6-chloro-8-fluoro-2-(((s)-1-methylpyrrolidin-2-yl)methoxy)quinazolin-4-yl)-3-methylpiperazin-1-yl)prop-2-en-1-one
Filed
2023-02-03
Issued
2026-03-03
Expires
2043-02-03
Fwd cites
0
Claims
40
Drawings
28
Drawings (3)
Agent Planner — multi-iter CAD reconstruction
No planner run yet. Click Run Planner → to start.
CAD Studio — AI 3D reconstruction
Synthesizing 3D model — Gemini vision → OpenSCAD → trimesh → PrusaSlicer (~30–60s)…
Abstract
Provided herein are salts and solid forms of 1-((S)-4-((R)-7-(6-amino-4-methyl-3-(trifluoromethyl)pyridin-2-yl)-6-chloro-8-fluoro-2-(((S)-1-methylpyrrolidin-2-yl)methoxy)quinazolin-4-yl)-3-methylpiperazin-1-yl)prop-2-en-1-one, including adipate, fumarate, ethylenesulphonate, besylate, and mesylate salts thereof.
Claims (40)
- 11. A crystal form comprising Compound A, Form A: having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 9.6474, 11.0365, 15.4059, 16.4193, and 18.7038 (±0.1° 2θ).
- 22. The crystal form of claim 1, wherein the crystal form of Compound A, Form A has an X-ray powder diffraction pattern comprising at least 15 additional characteristic X-ray powder diffraction peaks using CuKα radiation at 4.8059, 7.506, 8.5157, 9.2973, 11.1828, 11.677, 12.7936, 14.5086, 16.1353, 16.6719, 16.9847, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828 (±0.1° 2θ).
- 33. The crystal form of claim 1, wherein the crystal form of Compound A, Form A has an X-ray powder diffraction pattern comprising at least 10 additional characteristic X-ray powder diffraction peaks using CuKα radiation at 4.8059, 7.506, 8.5157, 9.2973, 11.1828, 11.677, 12.7936, 14.5086, 16.1353, 16.6719, 16.9847, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828 (±0.1°2θ).
- 44. The crystal form of claim 1, wherein the crystal form of Compound A, Form A has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 22.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, and 22.1828 (±0.1° 2θ) and comprising corresponding d-spacings at 18.37243 11.76829, 10.37514, 9.50454, 9.16041, 8.01034, 7.90589, 7.57235, 6.91391, 6.10025, 5.7469, 5.48871, 5.3944, 4.31324, 5.21609, 4.74037, 4.68829, 4.57458, 4.49117, 4.44156, 4.32518, 4.19755, 4.13611, 4.04295, and 4.00415 ([Å]).
- 55. The crystal form of claim 1, wherein the crystal form of Compound A, Form A has a weight loss of about 2% up to 100° C. as measured by TGA thermograph and two endotherms at 68.8° C. and 169.1° C. as measured by DSC thermograph.
- 66. A pharmaceutical composition comprising the solid form of claim 1 and at least one pharmaceutically acceptable excipient.
Description (36,836 words)
CROSS REFERENCE TO RELATED APPLICATIONS
This application claims the benefit of U.S. Provisional Patent Application No. 63/307,526, filed 7 Feb. 2022, and is incorporated herein by reference in its entirety and for all purposes.
FIELD OF THE INVENTION
Provided herein are solid forms of 1-((S)-4-((R)-7-(6-amino-4-methyl-3-(trifluoromethyl)pyridin-2-yl)-6-chloro-8-fluoro-2-(((S)-1-methylpyrrolidin-2-yl)methoxy)quinazolin-4-yl)-3-methylpiperazin-1-yl)prop-2-en-1-one and methods of their use in the treatment of cancer.
BACKGROUND
Compounds and pharmaceutically acceptable salts thereof described herein are useful in the treatment of various types of cancers, including for example, lung cancer and colorectal cancer.
It is not possible to predict whether a given molecule will crystallize in one or several crystal forms, whether it will form solvates with different stoichiometries or will combine with other molecules and form stable co-crystals. (Struct Bond (2009) 132: 25-50, 27). The relative stability of varying crystal forms and, for example, the possibility of interconversion between forms or between an amorphous phase and a crystalline phase can significantly and unpredictably affect both physical and chemical properties. Thus, altering the processing, stability, bioavailability, formulation, and/or storage of pharmaceutical compounds. There is no reliable predictability of the solid form and its usefulness as a crystalline solid or amorphous solid.
Accordingly, there is a need for identifying and isolating stable forms of 1-((S)-4-((R)-7-(6-amino-4-methyl-3-(trifluoromethyl)pyridin-2-yl)-6-chloro-8-fluoro-2-(((S)-1-methylpyrrolidin-2-yl)methoxy)quinazolin-4-yl)-3-methylpiperazin-1-yl)prop-2-en-1-one.
SUMMARY
Provided herein are solutions to the problems above and other problems in the art.
In one aspect provided herein is a compound of formula 1 as described herein.
In another aspect provided herein is a solid form of the compound of formula 1. In one embodiment, the solid for is Compound A. In one embodiment, the solid for is Compound B. In one embodiment, the solid form is Compound C. In one embodiment, the solid form is Compound D. In one embodiment, the solid form is Compound E. In one embodiment, the solid form is Compound F.
In another aspect provided herein is a solid form of Compound A corresponding to Compound A Form A as described herein. In one embodiment, is a solid form of Compound A corresponding to Compound A Form B as described herein. In one embodiment, is a solid form of Compound A corresponding to Compound A Form C as described herein. In one embodiment, is a solid form of Compound A corresponding to Compound A Form D as described herein.
In another aspect provided herein is a solid form of Compound B corresponding to Compound B Form A. Further provided herein is a solid form of Compound C corresponding to Compound C Form A. Further provided herein is a solid form of Compound D corresponding to Compound D Form A. Further provided herein is a solid form of Compound E corresponding to Compound E Form A. Further provided herein is a solid form of Compound F corresponding to Compound F Form A.
In another aspect provided herein is a method of treating a cancer comprising a KRasG12C mutation in a patient having said cancer, the method comprising administering an effective amount of Compound 1 as described herein or a crystal form corresponding to a Form as described herein of Compound A, Compound B, Compound C, Compound D, Compound E, or Compound F as described herein.
In still another aspect provided herein is a method of treating a cancer comprising a KRasG12C mutation in a patient having said cancer, the method comprising determining if the patient has the mutation and if the patient is determined to have the mutation, then administering an effective amount of Compound 1 as described herein or a crystal form corresponding to a Form as described herein of Compound A, Compound B, Compound C, Compound D, Compound E, or Compound F as described herein.
The present embodiments can be understood more fully by reference to the detailed description and examples, which are intended to exemplify non-limiting embodiments.
BRIEF DESCRIPTION OF THE FIGURES
FIG. 1 depicts the XRPD spectrum of Compound A Form A.
FIG. 2 depicts a TGA thermogram and DSC thermogram overlap for Compound A Form A.
FIG. 3 depicts a DSC thermogram for Compound A Form A.
FIG. 4 depicts single crystal XRD of Compound A Form A.
FIG. 5 depicts the XRPD spectrum of Compound A Form B.
FIG. 6 depicts a TGA thermogram and DSC thermogram overlap for Compound A Form B.
FIG. 7 depicts single crystal XRD of Compound A Form C.
FIG. 8 depicts the XRPD spectrum of Compound A Form D.
FIG. 9 depicts DSC thermogram for Compound A Form D.
FIG. 10 depicts a TGA thermogram and DSC thermogram overlap for Compound A Form D.
FIG. 11 depicts the XRPD spectrum overlay of Compound B Form A.
FIG. 12 depicts DSC thermogram for Compound B Form A.
FIG. 13 depicts the XRPD spectrum overlay of Compound C Form A.
FIG. 14 depicts a TGA thermogram and DSC thermogram overlap for Compound C Form A.
FIG. 15 depicts the XRPD spectrum overlay of Compound D Form A.
FIG. 16 depicts a TGA thermogram and DSC thermogram overlap for Compound D Form A.
FIG. 17 depicts the XRPD spectrum overlay of Compound E Form A.
FIG. 18 depicts the XRPD overlay of slurry competition between Compound A Form A and B.
FIG. 19 depicts XRPD of Compound A at varying relative humidity (RH).
FIG. 20 depicts single crystal XRD of Compound A Form D.
FIG. 21 depicts a view of the crystal packing of Compound A Form D looking down the crystallographic b-axis.
FIG. 22 depicts a view of the crystal packing of Compound A Form D looking down the crystallographic c-axis.
FIG. 23 depicts a view of the crystal packing of Form C looking down the crystallographic b-axis. Only major components of disorder are shown.
FIG. 24 depicts a view of the crystal packing of Form C looking down the crystallographic c-axis. Only major components of disorder are shown.
FIG. 25 depicts a comparison of crystal packing between hydrated Form D and anhydrous Form C, viewed down crystallographic b-axis.
FIG. 26 depicts the XRPD spectrum overlay of Compound F Form A.
FIG. 27 depicts a TGA thermogram and DSC thermogram overlap for Compound F Form A.
DETAILED DESCRIPTION
Unless defined otherwise, all technical and scientific terms used herein have the same meaning as commonly understood by those of ordinary skill in the art to which the invention belongs. See, e.g., Singleton et al., DICTIONARY OF MICROBIOLOGY AND MOLECULAR BIOLOGY 2nd ed., J. Wiley & Sons (New York, N.Y. 1994); Sambrook et al., MOLECULAR CLONING, A LABORATORY MANUAL, Cold Springs Harbor Press (Cold Springs Harbor, N Y 1989). Any methods, devices and materials similar or equivalent to those described herein can be used in the practice of this invention.
The following definitions are provided to facilitate understanding of certain terms used frequently herein and are not meant to limit the scope of the present disclosure. All references referred to herein are incorporated by reference in their entirety.
As used herein, and unless otherwise specified, the terms “about” and “approximately,” when referring to doses, amounts, or weight percents of ingredients of a composition or a dosage form, mean a dose, amount, or weight percent that is recognized by one of ordinary skill in the art to provide a pharmacological effect equivalent to that obtained from the specified dose, amount, or weight percent. The equivalent dose, amount, or weight percent can be within 30%, 20%, 15%, 10%, 5%, 1%, or less of the specified dose, amount, or weight percent.
As used herein, and unless otherwise specified, the terms “about” and “approximately,” when referring to a numeric value or range of values used for characterization of a particular solid form described herein (e.g., XRPD peak values) indicate that the value or range of values may deviate from a given value to an extent deemed reasonable to one of ordinary skill in the art while still describing the solid form. In one embodiment, the value of an XRPD peak position may vary by up to ±0.1° 2θ (or ±0.05 degree 2θ) while still describing the particular XRPD peak.
As used herein, and unless otherwise specified, a crystalline that is “pure,” i.e., substantially free of other crystalline or amorphous solids or other chemical compounds, and contains less than about 10%, 9%, 8%, 7%, 6%, 5%, 4%, 3%, 2%, 1%, 0.5%, 0.4%, 0.3%, 0.2%, 0.1%, 0.05%, or 0.01% of one or more other solid forms on a weight basis. The detection of other solid forms can be accomplished by, for example, diffraction analysis, thermal analysis, elemental combustion analysis and/or spectroscopic analysis. The detection of other chemical compounds can be accomplished by, for example, mass spectrometry analysis, spectroscopic analysis, thermal analysis, elemental combustion analysis and/or chromatographic analysis.
Unless otherwise specified, the terms “solvate” and “solvated,” as used herein, refer to a solid form of a substance which contains solvent. The terms “hydrate” and “hydrated” refer to a solvate wherein the solvent is water. The terms “solvate” and “solvated,” as used herein, can also refer to a solvate of a salt, cocrystal, or molecular complex. The terms “hydrate” and “hydrated,” as used herein, can also refer to a hydrate of a salt, cocrystal, or molecular complex.
The term “pharmaceutically acceptable,” refers to a diluent, excipient, or carrier in a formulation compatible with the other ingredient(s) of the formulation and not deleterious to the recipient thereof.
“Compound 1” refers to a compound having the structure:
and having the name 1-((S)-4-((R)-7-(6-amino-4-methyl-3-(trifluoromethyl)pyridin-2-yl)-6-chloro-8-fluoro-2-(((S)-1-methylpyrrolidin-2-yl)methoxy)quinazolin-4-yl)-3-methylpiperazin-1-yl)prop-2-en-1-one.
“Compound A” refers to a compound having the structure:
In some embodiments, Compound A is also described as Compound 1 adipate.
“Compound B” refers to a compound having the structure:
In some embodiments, Compound B is also described as Compound 1 fumarate.
“Compound C” refers to a compound having the structure:
In some embodiments, Compound C is also described as Compound 1 ethylenesulphonate.
“Compound D” refers to a compound having the structure:
In some embodiments, Compound D is also described as Compound 1 besylate.
“Compound E” refers to a compound having the structure:
In some embodiments, Compound E is also described as Compound 1 mesylate.
“Compound F” refers to a compound having the structure:
In some embodiments, Compound F is also described as Compound 1 acetate.
The term “solid form” refers to a physical form that is not predominantly in a liquid or a gaseous state. A solid form may be a crystalline form or a mixture thereof. In certain embodiments, a solid form may be a liquid crystal. In certain embodiments, the solid form of Compound A is a solid form corresponding to Compound A Form A, Compound A Form B, Compound A Form C, Compound A Form D, Compound B Form A, Compound C Form A, Compound D Form A, or Compound E Form A, or Compound F Form A, or a mixture thereof.
In one embodiment, the solid form of Compound A is an adipate salt corresponding to Form A. In one embodiment, the solid form of Compound A is an adipate salt corresponding to Form B. In another embodiment, the solid form of Compound A is an adipate salt corresponding to Form C. In still another embodiment, the solid form of Compound A is an adipate salt corresponding to Form D. In one embodiment, the solid form of Compound B is a fumarate salt corresponding to Form A. In another embodiment, the solid form of Compound C is an ethylenesulphonate salt corresponding to Form A. In another embodiment, the solid form of Compound D is a besylate salt corresponding to Form A. In another embodiment, the solid form of Compound E is a mesylate salt corresponding to Form A. In another embodiment, the solid form Compound F is an acetate salt corresponding to Form A.
The term “crystal form” or “crystalline form” refers to a solid form that is crystalline. In certain embodiments, a crystal form of a compound described herein may be substantially free of amorphous solids and/or other crystal forms. In certain embodiments, a crystal form of a compound described herein may contain less than about 1%, less than about 2%, less than about 3%, less than about 4%, less than about 5%, less than about 6%, less than about 7%, less than about 8%, less than about 9%, less than about 10%, less than about 15%, less than about 20%, less than about 25%, less than about 30%, less than about 35%, less than about 40%, less than about 45%, or less than about 50% by weight of one or more amorphous solids and/or other crystal forms. In certain embodiments, a crystal form described herein is pure. In certain embodiments, a crystal form of a compound described herein may be about 99%, 98%, 97%, 96%, 95%, 94%, 93%, 92%, 91%, or 90% pure. In some embodiments, a crystal form is a solid form described herein.
The term “amorphous” or “amorphous solid” refers to a solid form that not substantially crystalline as determined by X-ray diffraction. In particular, the term “amorphous solid” describes a disordered solid form, i.e., a solid form lacking long range crystalline order. In certain embodiments, an amorphous solid of a compound described herein may be substantially free of other amorphous solids and/or crystal forms. In certain embodiments, an amorphous solid may be pure. In certain embodiments, an amorphous solid of a compound described herein may be about 99%, 98%, 97%, 96%, 95%, 94%, 93%, 92%, 91%, or 90% pure.
A “patient” or “subject” is defined herein to include animals, such as mammals, including, but not limited to, primates (e.g., humans), cows, sheep, goats, horses, dogs, cats, rabbits, rats, mice, monkeys, chickens, turkeys, quails, or guinea pigs and the like, in one embodiment a mammal, in another embodiment a human. In one embodiment, a subject is a human having or at risk for cancer.
As used herein, “essentially” refers to at least 90%, at least 95%, at least 98% or at least 99%.
In the description herein, if there is a discrepancy between a depicted structure and a name given to that structure, then the depicted structure controls. Additionally, if the stereochemistry of a structure or a portion of a structure is not indicated with, for example, bold wedged, or dashed lines, the structure or portion of the structure is to be interpreted as encompassing all stereoisomers of it. In some cases, however, where more than one chiral center exists, the structures and names may be represented as single enantiomers to help describe the relative stereochemistry.
Unless otherwise indicated, the terms “a compound of the formula” or “a compound of formula” or “compounds of the formula” or “compounds of formula” refer to any compound selected from the genus of compounds as defined by the formula (including any pharmaceutically acceptable salt of any such compound if not otherwise noted).
The terms “treat”, “treating”, and “treatment” refer to clinical intervention designed to alter the natural course of the patient or cell being treated during the course of clinical pathology. Desirable effects of treatment include decreasing the rate of disease progression, ameliorating or palliating the disease state, and remission or improved prognosis. For example, a patient is successfully “treated” if one or more symptoms associated with a cancer described herein are mitigated or eliminated, including, but are not limited to, reducing the proliferation of (or destroying) cancerous cells, decreasing symptoms resulting from the disease, increasing the quality of life of those suffering from the disease, decreasing the dose of other medications required to treat the disease, and/or prolonging survival of patients.
The term “delaying progression” of a disease refers to deferring, hindering, slowing, retarding, stabilizing, and/or postponing development of a cancer described herein. This delay can be of varying lengths of time, depending on the history of the cancer and/or patient being treated. As is evident to one skilled in the art, a sufficient or significant delay can, in effect, encompass prevention, in that the patient does not develop cancer.
An “effective amount” is at least the minimum amount required to effect a measurable improvement of a cancer described herein. An effective amount herein may vary according to factors such as the disease state, age, sex, and weight of the patient, and the ability of the agent to elicit a desired response in the patient. An effective amount is also one in which any toxic or detrimental effects of the treatment are outweighed by the therapeutically beneficial effects. Beneficial or desired results include results such as eliminating or reducing the risk, lessening the severity, delaying the onset of the disease (including biochemical, histological and/or behavioral symptoms of the disease, its complications and intermediate pathological phenotypes presenting during development of the disease), decreasing one or more symptoms resulting from the disease, increasing the quality of life of those suffering from the disease, decreasing the dose of other medications required to treat the disease, enhancing effect of another medication such as via targeting, delaying the progression of the disease, and/or prolonging survival. In some embodiments, an effective amount of the drug may have the effect in reducing the number of cancer cells; reducing the tumor size; inhibiting (i.e., slow or stop) cancer cell infiltration into peripheral organs; inhibit (i.e., slow or stop) tumor metastasis; inhibiting (i.e., slow or stop) tumor growth; and/or relieving one or more of the symptoms associated with the disorder. An effective amount can be administered in one or more administrations. An effective amount of drug, compound, pharmaceutical composition, or combination therapy described herein can be an amount sufficient to accomplish therapeutic treatment either directly or indirectly. As is understood in the clinical context, an effective amount of a drug, compound, or pharmaceutical composition may or may not be achieved in conjunction with another drug, compound, or pharmaceutical composition, or combination therapy. Thus, an “effective amount” may be considered in the context of administering one or more therapeutic agents, and a single agent may be considered to be given in an effective amount if, in conjunction with one or more other agents, a desirable result may be or is achieved.
Exemplary solvent abbreviations used herein
Abbre-
Abbre-
viation
Solvent
viation
Solvent
MeOH
Methanol
ACN
Acetonitrile
EtOH
Ethanol
DCM
Dichloromethane
IPA
Isopropyl alcohol
EtOAc
Ethyl acetate
MIBK
Methyl isobutyl ketone
IPAc
Isopropyl acetate
MEK
Methyl ethyl ketone
2-MeTHF
2-Methyltetrahydrofuran
NMP
N-Methyl pyrrolidone
THF
Tetrahydrofuran
DMF
Dimethyl formamide
DMSO
Dimethyl sulfoxide
CPME
Cyclopentyl methyl ether
DMAc
Dimethylacetamide
MTBE
Methyl tert-butyl ether
—
—
Polymorphs
Provided herein are solid forms, formulations comprising such solid forms, and methods of using such solid forms of Compound 1 (e.g. Compound A, B, C, D, or E). In one embodiment provided herein are solid forms of Compound 1. Compound 1 can be a freebase as described herein existing in an amorphous solid form.
In one embodiment, Compound 1 is a crystalline adipate salt having the formula of Compound A as described herein. In one embodiment, Compound A exists in one or more forms as described herein. In one such embodiment, Compound A comprises Compound A Form A as described herein. In one such embodiment, Compound A comprises Compound A Form B as described herein. In one such embodiment, Compound A comprises Compound A Form C as described herein. In one such embodiment, Compound A comprises Compound A Form D as described herein. In another such embodiment, Compound A consists of a single Form (e.g. A, B, C, D) as described herein. In one embodiment, a compound or pharmaceutical composition described herein comprises two or more forms of Compound A. In one such embodiment, the compound or pharmaceutically acceptable salt thereof described herein comprises a mixture of Compound A Form A and Compound A Form D as described herein. In one embodiment, the compound or pharmaceutically acceptable salt thereof described herein comprises a mixture of Compound A Form A and Compound A Form C as described herein.
In another embodiment, Compound 1 is a crystalline fumarate salt having the formula of Compound B as described herein. In one such embodiment, Compound B comprises Compound B Form A as described herein.
In another embodiment, Compound 1 is a crystalline ethylenesulphonate salt having the formula of Compound C as described herein. In one such embodiment, Compound C comprises Compound C Form A as described herein.
In another embodiment, Compound 1 is a crystalline besylate salt having the formula of Compound D as described herein. In one such embodiment, Compound D comprises Compound D Form A as described herein.
In another embodiment, Compound 1 is a crystalline mesylate salt having the formula of Compound E as described herein. In one such embodiment, Compound E comprises Compound E Form A as described herein.
In another embodiment, Compound 1 is a crystalline acetate salt having the formula of Compound F as described herein. In one such embodiment, Compound F comprises Compound F Form A as described herein.
Solid forms can be characterized by physical properties such as, for example, stability, solubility and dissolution rate, density, compressibility, hardness, morphology, cleavage, stickiness, solubility, water uptake, electrical properties, thermal behavior, solid-state reactivity, physical stability, and chemical stability) affecting particular processes (e.g., yield, filtration, washing, drying, milling, mixing, tableting, flowability, dissolution, formulation, and lyophilization) which make certain solid forms suitable for the manufacture of a solid dosage form. Such properties can be determined using particular analytical chemical techniques, including solid-state analytical techniques (e.g., X-ray diffraction, microscopy, spectroscopy and thermal analysis), as described herein and are unpredictable. There is no protocol of polymorph screening that can guarantee the identification of all crystal forms of a given molecule.
Techniques for characterizing crystal forms and amorphous solids include, for example, thermal analysis (e.g., differential scanning calorimetry (DSC), dynamic vapor sorption (DVS), thermal gravimetric analysis (TGA), and hot-stage microscopy), spectroscopy (e.g., infrared, Raman, and solid-state nuclear magnetic resonance), differential scanning calorimetry (DSC), X-ray powder diffractometry (XRPD), single-crystal X-ray diffractometry, vibrational spectroscopy, e.g., infrared (IR) and Raman spectroscopy, solid-state and solution nuclear magnetic resonance (NMR) spectroscopy (including 1H NMR and F NMR), scanning electron microscopy (SEM), electron crystallography and quantitative analysis, particle size analysis (PSA), surface area analysis, solubility studies, and dissolution studies, ultra-high performance liquid chromatography (UHPLC), and proton nuclear magnetic resonance spectrum.
The purity of the solid forms provided herein can be determined by standard analytical methods, such as thin layer chromatography (TLC), gel electrophoresis, gas chromatography, ultra-high performance liquid chromatography (UHPLC), and mass spectrometry (MS).
Compound A: Form A
In some embodiments, provided herein is a solid form corresponding to Compound A designated as Form A. Form A is an adipate crystalline solid form of Compound 1. In one embodiment, Form A of Compound A is an anhydrate. In one embodiment, Form A of Compound A is obtained from acetone, THF, or EtOAc. In one embodiment, Form A of Compound A is obtained from acetone. In another embodiment, Form A of Compound A is obtained from THF. In another embodiment, Form A of Compound A is obtained from EtOAc. In one embodiment, the stoichiometric ratio of adipic acid:freebase of Form A of Compound A is 0.9, 1.0, 1.01, 1.02, 1.03, 1.04, 1.05, 1.06, 1.07, 1.08, 1.09, or 1.10. In one such embodiment, the stoichiometric ratio of adipic acid:freebase of Form A of Compound A is 1.06.
In one embodiment, a solid form provided herein, e.g., Form A of Compound A, is a adipate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form A of Compound A, is substantially as shown in FIG. 1. In another embodiment, a solid form provided herein, e.g., Form A of Compound A, has one or more characteristic XRPD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 3, 5, 10, 15, or 20 characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least five, six, seven, eight, nine, ten, eleven, twelve, thirteen, fourteen, fifteen, sixteen, seventeen, eighteen, nineteen, twenty, or all of the characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 10 characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 9.6474, 11.0365, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 18.7038, 18.9135, or 21.9673±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 5 characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 1, 2, 3, 4, or 5 characteristic XPRD peaks at approximately 9.6474, 11.0365, 15.4059, 16.4193, 18.7038±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In one embodiment, a solid form provided herein, e.g., Form A of Compound A, comprises an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 9.6474, 11.0365, 15.4059, 16.4193, 18.7038 (±0.1° 2θ).
In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 15 characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has at least 20 characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, or 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound A, has all of the characteristic XPRD peaks at approximately 4.8059, 7.506, 8.5157, 9.2973, 9.6474, 11.0365, 11.1828, 11.677, 12.7936, 14.5086, 15.4059, 16.1353, 16.4193, 16.6719, 16.9847, 18.7038, 18.9135, 19.3881, 19.7517, 19.9746, 20.5178, 21.1487, 21.4666, 21.9673, and 22.1828±0.1° 2θ, as depicted in, for example, FIG. 1, and as found in Table 1 herein.
TABLE 1
Representative XRPD Peaks for Compound A Form A
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
4.8059
18.37243
12.57
7.506
11.76829
20.27
8.5157
10.37514
6.82
9.2973
9.50454
22.86
9.6474
9.16041
85.05
11.0365
8.01034
57.73
11.1828
7.90589
25.7
11.677
7.57235
11.66
12.7936
6.91391
20.85
14.5086
6.10025
33.73
15.4059
5.7469
100
16.1353
5.48871
40.28
16.4193
5.3944
65.37
16.6719
5.31324
30.23
16.9847
5.21609
18.22
18.7038
4.74037
89.52
18.9135
4.68829
39.33
19.3881
4.57458
19.09
19.7517
4.49117
10.64
19.9746
4.44156
24.31
20.5178
4.32518
24.85
21.1487
4.19755
25.86
21.4666
4.13611
9.25
21.9673
4.04295
43.19
22.1828
4.00415
20.22
In one embodiment described herein, Form A of Compound A has a TGA thermogram as substantially depicted in FIG. 2, comprising a weight loss of about 2% up to 100° C.
In one such embodiment, Form A of Compound A has a DSC thermogram corresponding to FIG. 2, comprising two endotherms at 68.8° C. and 169.1° C.
In one embodiment, Form A of Compound A has a DSC thermogram corresponding to FIG. 3, comprising one endotherm at 173.3° C. (peak).
Single crystal XRD for Compound A Form A is shown in FIG. 4. Absolute stereochemistry was unambiguously determined from the diffraction data and is depicted in FIG. 4.
Compound A: Form B
In some embodiments, provided herein is a solid form corresponding to Compound A designated as Form B. Form B is a crystalline solid form of Compound A. In one embodiment, Form B of Compound A is obtained from anti-solvent addition in DCM/toluene, followed by transferring to 5° C. In one embodiment, Form B of Compound A is an anhydrate. In one embodiment, no form change is observed after air drying at RT overnight. In one embodiment, the stoichiometric ratio of adipic acid:freebase of Form B of Compound A is 1.5, 1.55, 1.6, 1.65, 1.7, 1.8, 1.9, 2, 2.05, or 2.10. In one embodiment, the stoichiometric ratio of adipic acid:freebase of Form B of Compound A is 1.65 or 2.10.
In one embodiment, a solid form provided herein, e.g., Form B of Compound A, is a adipate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form B of Compound A, is substantially as shown in FIG. 5. In another embodiment, a solid form provided herein, e.g., Form B of Compound A, has one or more characteristic XRPD peaks at approximately 5.2063, 8.8524, 11.1301, 12.3721, 14.63, 15.6885, 17.7161, 18.2857, 19.8008, 21.9253, or 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein. In another embodiment, a solid form provided herein, e.g., Form B of Compound A, has at least 3, 5, 7, 9, or 10 characteristic XPRD peaks at approximately 5.2063, 8.8524, 11.1301, 12.3721, 14.63, 15.6885, 17.7161, 18.2857, 19.8008, 21.9253, or 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein. In still another embodiment, a solid form provided herein, e.g., Form B of Compound A, has at least 5, 6, 7, 8, 9, 10 or all of the characteristic XPRD peaks at approximately 5.2063, 8.8524, 11.1301, 12.3721, 14.63, 15.6885, 17.7161, 18.2857, 19.8008, 21.9253, or 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein.
In still another embodiment, a solid form provided herein, e.g., Form B of Compound A, has at least 10 characteristic XPRD peaks at approximately 5.2063, 8.8524, 11.1301, 12.3721, 14.63, 15.6885, 17.7161, 18.2857, 19.8008, 21.9253, or 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein. In another embodiment, a solid form provided herein, e.g., Form B of Compound A, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 5.2063, 8.8524, 12.3721, 14.63, 15.6885, 17.7161, 18.2857, 19.8008, 21.9253, or 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein.
In still another embodiment, a solid form provided herein, e.g., Form B of Compound A, has at least 5 characteristic XPRD peaks at approximately 5.2063, 8.8524, 11.1301, 12.3721, 14.63, 15.6885, 17.7161, 18.2857, 19.8008, 21.9253, or 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein. In still another embodiment, a solid form provided herein, e.g., Form B of Compound A, has at least 1, 2, 3, 4, or 5 characteristic XPRD peaks at approximately 5.2063, 14.63, 17.7161, 21.9253, 25.1335±0.1° 2θ, as depicted in, for example, FIG. 5, and as found in Table 2 herein. In one embodiment, a solid form provided herein, e.g., Form B of Compound A, has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 5.2063, 14.63, 17.7161, 21.9253, 25.1335 (±0.1° 2θ).
TABLE 2
Representative XRPD Peaks for Compound A Form B
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
5.2063
16.96012
100
8.8524
9.98124
13.93
11.1301
7.94318
12.92
12.3721
7.14847
19.39
14.63
6.04991
31.95
15.6885
5.64402
18.78
17.7161
5.00236
19.59
18.2857
4.84781
18.68
19.8008
4.48015
15.37
21.9253
4.0506
22.24
25.1335
3.54035
22.89
In one embodiment described herein, Form B of Compound A has a TGA thermogram as substantially depicted in FIG. 6, comprising a weight loss of about 2.2% up to 100° C. No form change may be observed after heating Form B of Compound A under nitrogen to about 90° C.
In one such embodiment, Form B of Compound A has a DSC thermogram corresponding to FIG. 6, comprising two broad endotherms at 55.7° C. and 109.6° and a small end other at 158.8° C.
Compound A: Form C
In some embodiments, provided herein is a solid form corresponding to Compound A designated as Form C. Form C is a crystalline solid form of Compound A. In one embodiment, Form C of Compound A is an anhydrate. In one such embodiment, Form C of Compound A is an under-occupied variant of Form D. In one embodiment, Form C is a disordered lattice when compared to Form A or Form D of Compound A. In another such embodiment, the asymmetric unit contains one molecule of Compound A with positionally disordered methylpyrrolidine ring and one adipate anion with one COO— group disordered over two sites (approximately 50/50). (See Examples below). In one embodiment, Form C of Compound A is formed by dehydrating Form D of Compound A. In one such embodiment, the percentage of Form D of Compound A after drying is less than 20%, 15%, 12%, 10%, 8%, 6%, 5%, 2%, or 1%.
In one embodiment, a solid form provided herein, e.g., Form C of Compound A, is a adipate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form C of Compound A, is equivalent to Form A of Compound A.
Single Crystal XRD of Compound A Form C is shown in FIG. 7.
Compound A: Form D
In some embodiments, provided herein is a solid form corresponding to Compound A designated as Form D. Form D is a crystalline solid form of Compound B. In one embodiment, Form D of Compound A is a hemihydrate. In one embodiment, Form D of Compound A is formed by exposing Form A or Form C of Compound A as described herein to increasing percentage of relative humidity (rh). In one embodiment, Form D can be dried, thereby reforming Form A and/or Form C of Compound A. In one such embodiment, the percentage of Form D of Compound A after drying is less than 20%, 15%, 12%, 10%, 8%, 6%, 5%, 2%, or 1%.
In one embodiment, a solid form provided herein, e.g., Form D of Compound A, is a adipate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form D of Compound A, is substantially as shown in FIG. 8. In another embodiment, a solid form provided herein, e.g., Form D of Compound A, has one or more characteristic XRPD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein. In another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 3, 5, 10, 15, or 20 characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein. In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 14, 15, 16, 17, 18, 19, 20, or all of the characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein.
In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 10 characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein. In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 15.2452, 11.0487, 18.6477, 18.7908, 9.7745, 11.2178, 16.6345, 16.0821, 16.3536, or 20.6308±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein.
In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 5 characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein. In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 1, 2, 3, 4, or 5 characteristic XPRD peaks at approximately 9.7745, 11.0487, 15.2452, 18.6477, 18.7908±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein. In one embodiment, a solid form provided herein, e.g., Form D of Compound A, has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 9.7745, 11.0487, 15.2452, 18.6477, 18.7908 (±0.1° 2θ)
In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 15 characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein.
In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has at least 20 characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein.
In still another embodiment, a solid form provided herein, e.g., Form D of Compound A, has all of the characteristic XPRD peaks at approximately 7.4529, 9.309, 9.7745, 11.0487, 11.2178, 11.6936, 12.8642, 14.65, 14.9254, 15.2452, 15.5252, 16.0821, 16.3536, 16.6345, 17.1089, 17.3151, 18.6477, 18.7908, 19.5758, 19.8874, 20.2, 20.6308, 21.0403, 21.6587, or 22.0397±0.1° 2θ, as depicted in, for example, FIG. 8, and as found in Table 3 herein.
In one embodiment, the single crystal XRD of Compound A Form D is provided in FIG. 21. Crystal packing and other scXRD information for Compound A Form D is as set forth herein (e.g. Examples).
TABLE 3
Representative XRPD Peaks for Compound A Form
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
7.4529
11.85207
17.22
9.309
9.49265
24.32
9.7745
9.04158
56.55
11.0487
8.00156
64.53
11.2178
7.88129
55.85
11.6936
7.56169
20.16
12.8642
6.87607
13.15
14.65
6.04167
18.46
14.9254
5.93083
7.53
15.2452
5.80712
100
15.5252
5.70301
16.24
16.0821
5.50675
46.63
16.3536
5.41595
41.59
16.6345
5.32509
52.84
17.1089
5.17852
12.68
17.3151
5.11731
9.61
18.6477
4.75451
62.88
18.7908
4.71863
58.63
19.5758
4.53114
16.41
19.8874
4.46084
14.43
20.2
4.39251
32.41
20.6308
4.30174
41.35
21.0403
4.21895
30.63
21.6587
4.09985
15.45
22.0397
4.02983
35.46
In one embodiment described herein, Compound A Form D has a DSC thermogram as substantially depicted in FIG. 9. In one embodiment, the DSC of Compound A Form D has one endotherm at about 173.4° C. (Peak).
In one embodiment described herein, Form B of Compound A has a TGA thermogram as substantially depicted in FIG. 10, comprising a weight loss of about 1.4% up to 100° C.
Compound B: Form A
In some embodiments, provided herein is a solid form corresponding to Compound B designated as Form A. Compound B Form A is a fumarate crystalline solid form of Compound B. In one embodiment, Compound B Form A is obtained from acetone and air dried at RT. In one embodiment, Compound B Form A is an anhydrate.
In one embodiment, no form change was observed before and after heating Compound B Form A to 100° C. under N2 protection and cooling down and exposed to ambient conditions.
In one embodiment, a solid form provided herein, e.g., Form A of Compound B, is a fumarate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form A of Compound B, is substantially as shown in FIG. 11. In another embodiment, a solid form provided herein, e.g., Form A of Compound B, has one or more characteristic XRPD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein. In another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 3, 5, 10, 15, or 20 characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, or all of the characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 10 characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 6.6796, 13.3393, 14.9097, 15.2963, 17.4837, 19.4416, 20.3394, 23.0009, 23.7124, or 26.7708±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 5 characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 1, 2, 3, 4, or 5 characteristic XPRD peaks at approximately 6.6796, 14.9097, 15.2963, 19.4416, 23.7124±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein. In one embodiment, a solid form provided herein, e.g., Form A of Compound B, has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 6.6796, 14.9097, 15.2963, 19.4416, 23.7124 (±0.1° 2θ).
In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 15 characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has at least 20 characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, or 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound B, has all of the characteristic XPRD peaks at approximately 6.6796, 7.8754, 8.4472, 8.724, 9.6832, 12.1433, 13.3393, 14.1386, 14.9097, 15.2963, 17.4837, 18.5763, 19.4416, 20.3394, 21.4642, 22.4341, 23.0009, 23.3901, 23.7124, 24.7816, 26.1995, 26.7708, 27.7302, and 30.9939±0.1° 2θ, as depicted in, for example, FIG. 11, and as found in Table 4 herein.
TABLE 4
Representative XRPD Peaks for Compound B Form A
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
6.6796
13.22236
43.06
7.8754
11.21714
22.02
8.4472
10.45905
13.58
8.724
10.12778
20.88
9.6832
9.1266
22.35
12.1433
7.28262
25.77
13.3393
6.63225
31.01
14.1386
6.25903
12.07
14.9097
5.93701
77.21
15.2963
5.78782
100
17.4837
5.06834
27
18.5763
4.77263
21.29
19.4416
4.5621
66.36
20.3394
4.36271
34.81
21.4642
4.13656
6.92
22.4341
3.95988
12.22
23.0009
3.86356
31.5
23.3901
3.80014
25.7
23.7124
3.74921
52.37
24.7816
3.58982
13.39
26.1995
3.39867
10
26.7708
3.32742
27.07
27.7302
3.21445
12.56
30.9939
2.883
11.13
In one embodiment described herein, Form A of Compound B has a DSC thermogram as substantially depicted in FIG. 12.
In one such embodiment, the DSC thermogram comprises one endotherm at about 58.7° C. and an overlapped peak with peak temperature at 157.1° C.
In another embodiment, Form A of Compound B is pure. In one such embodiment, Form A of Compound B is substantially free of other solid forms described herein (e.g. amorphous solid). In another embodiment, the purity of Form A of Compound B is no less than about 95%, no less than about 96%, no less than about 97%, no less than about 98%, no less than about 99%, no less than about 99.5%, or no less than about 99.9%.
Compound C: Form A
In some embodiments, provided herein is a solid form corresponding to Compound C designated as Form A. Form A of Compound C is a ethylsulphonate crystalline solid form of Compound C. In one embodiment, Form A of Compound C is obtained from ethyl acetate and air dried at RT.
In one embodiment, no form change was observed before and after heating Form A of Compound C to 100° C. under N2 protection and cooling down and exposed to ambient conditions.
In one embodiment, a solid form provided herein, e.g., Form A of Compound C, is an ethylenesulphonate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form A of Compound C, is substantially as shown in FIG. 13. In another embodiment, a solid form provided herein, e.g., Form A of Compound C, has one or more characteristic XRPD peaks at approximately 5.5814, 8.7554, 11.1932, 12.5401, 13.5091, 14.2557, 15.8682, 16.3963, 16.834, 17.5707, 18.9739, 20.2549, 21.3525, 26.5569±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein. In another embodiment, a solid form provided herein, e.g., Form A of Compound C, has at least 3, 5, 7, 10, or 12 characteristic XPRD peaks at approximately 5.5814, 8.7554, 11.1932, 12.5401, 13.5091, 14.2557, 15.8682, 16.3963, 16.834, 17.5707, 18.9739, 20.2549, 21.3525, 26.5569±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound C, has at least 5, 6, 7, 8, 9, 10, 11, 12, 13, or all of the characteristic XPRD peaks at approximately 5.5814, 8.7554, 11.1932, 12.5401, 13.5091, 14.2557, 15.8682, 16.3963, 16.834, 17.5707, 18.9739, 20.2549, 21.3525, 26.5569±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound C, has at least 10 characteristic XPRD peaks at approximately 5.5814, 8.7554, 11.1932, 12.5401, 13.5091, 14.2557, 15.8682, 16.3963, 16.834, 17.5707, 18.9739, 20.2549, 21.3525, 26.5569±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound C, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 12.5401, 17.5707, 16.834, 21.3525, 26.5569, 8.7554, 14.2557, 16.3963, 20.2549, 11.1932±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound C, has at least 5 characteristic XPRD peaks at approximately 5.5814, 8.7554, 11.1932, 12.5401, 13.5091, 14.2557, 15.8682, 16.3963, 16.834, 17.5707, 18.9739, 20.2549, 21.3525, 26.5569±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound C, has at least 5 characteristic XPRD peaks at approximately 12.5401, 17.5707, 16.834, 21.3525, 26.5569±0.1° 2θ, as depicted in, for example, FIG. 13, and as found in Table 5 herein. In one embodiment, a solid form provided herein, e.g., Form A of Compound C, has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 12.5401, 17.5707, 16.834, 21.3525, 26.5569 (±0.1° 2θ).
TABLE 5
Representative XRPD Peaks for Compound C Form A
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
5.5814
15.82116
18.18
8.7554
10.09154
27.49
11.1932
7.89859
22.06
12.5401
7.05308
100
13.5091
6.54927
10.14
14.2557
6.2079
26.79
15.8682
5.58052
19.33
16.3963
5.40194
25.03
16.834
5.26244
71.34
17.5707
5.04343
73.89
18.9739
4.67349
21.79
20.2549
4.38072
23.49
21.3525
4.15796
32.57
26.5569
3.35374
31.51
In one embodiment described herein, Form A of Compound C has a TGA thermogram as substantially depicted in FIG. 14. In one embodiment, a weight loss of 8.6% up to 100° C. is observed.
In one embodiment, Form A of Compound C has a DSC thermogram as substantially depicted in FIG. 14, comprising two endotherms at 81.0° C. and 149.2° C. (peak temperature).
In another embodiment, Form A of Compound C is pure. In one such embodiment, Form A of Compound C is substantially free of other solid forms described herein (e.g. amorphous solid). In another embodiment, the purity of Form A of Compound C is no less than about 95%, no less than about 96%, no less than about 97%, no less than about 98%, no less than about 99%, no less than about 99.5%, or no less than about 99.9%.
Compound D: Form A
In some embodiments, provided herein is a solid form corresponding to Compound D designated as Form A. Form A of Compound D is a crystalline solid form of Compound D. In one embodiment, Form A of Compound D is obtained from evaporation of acetone/n-heptane (1:1 v/v).
In one embodiment, a solid form provided herein, e.g., Form A of Compound D, is an besylate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form A of Compound D, is substantially as shown in FIG. 15. In another embodiment, a solid form provided herein, e.g., Form A of Compound D, has one or more characteristic XRPD peaks at approximately 7.3809, 9.2213, 10.7407, 12.7588, 13.6799, 14.654, 15.8145, 17.1195, 18.5979, 19.5937, 20.8941, 21.9068, 24.4114, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein. In another embodiment, a solid form provided herein, e.g., Form A of Compound D, has at least 3, 5, 7, 10 or 12 characteristic XPRD peaks at approximately 7.3809, 9.2213, 10.7407, 12.7588, 13.6799, 14.654, 15.8145, 17.1195, 18.5979, 19.5937, 20.8941, 21.9068, 24.4114, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound D, has at least 5, 6, 7, 8, 9, 10, 11, 12, 13, or all of the characteristic XPRD peaks at approximately 7.3809, 9.2213, 10.7407, 12.7588, 13.6799, 14.654, 15.8145, 17.1195, 18.5979, 19.5937, 20.8941, 21.9068, 24.4114, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound D, has at least 10 characteristic XPRD peaks at approximately 7.3809, 9.2213, 10.7407, 12.7588, 13.6799, 14.654, 15.8145, 17.1195, 18.5979, 19.5937, 20.8941, 21.9068, 24.4114, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound D, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 7.3809, 10.7407, 12.7588, 14.654, 15.8145, 17.1195, 18.5979, 21.9068, 24.4114, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound D, has at least 5 characteristic XPRD peaks at approximately 7.3809, 9.2213, 10.7407, 12.7588, 13.6799, 14.654, 15.8145, 17.1195, 18.5979, 19.5937, 20.8941, 21.9068, 24.4114, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound D, has at least 5 characteristic XPRD peaks at approximately 7.3809, 10.7407, 14.654, 18.5979, 25.2558±0.1° 2θ, as depicted in, for example, FIG. 15, and as found in Table 6 herein. In one embodiment, a solid form provided herein, e.g., Form A of Compound D, has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 7.3809, 10.7407, 14.654, 18.5979, 25.2558 (±0.1° 2θ).
TABLE 6
Representative XRPD Peaks for Compound D Form A
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
7.3809
11.96741
100
9.2213
9.58275
1.19
10.7407
8.23033
18.04
12.7588
6.93266
8.47
13.6799
6.46789
2.68
14.654
6.04005
34.95
15.8145
5.59932
3.01
17.1195
5.17532
3.34
18.5979
4.76713
15.98
19.5937
4.52704
1.74
20.8941
4.24813
2.07
21.9068
4.05397
12.77
24.4114
3.64343
10.56
25.2558
3.52348
15.68
In one embodiment described herein, Form A of Compound D has a TGA thermogram as substantially depicted in FIG. 16. In one embodiment, a weight loss of 7.7% was observed up to 170° C. is observed.
In one embodiment, Form A of Compound D has a DSC thermogram as substantially depicted in FIG. 16, comprising one endotherm at 75.8° C. In one embodiment, the stoichiometric ratio of benzenesulfonic acid:freebase is 1, 1.01, 1.02, or 1.03.
In another embodiment, Form A of Compound D is pure. In one such embodiment, Form A of Compound D is substantially free of other solid forms described herein (e.g. amorphous solid). In another embodiment, the purity of Form A of Compound D is no less than about 95%, no less than about 96%, no less than about 97%, no less than about 98%, no less than about 99%, no less than about 99.5%, or no less than about 99.9%.
Compound E: Form A
In some embodiments, provided herein is a solid form corresponding to Compound E designated as Form A. Form A of Compound E is a crystalline solid form of Compound E. In one embodiment, Form A of Compound E is obtained from acetone.
In one embodiment, a solid form provided herein, e.g., Form A of Compound E, is an mesylate salt, and is substantially crystalline, as indicated by X-ray powder diffraction pattern (XRPD) measurements. In one embodiment, the XRPD of a solid form provided herein, e.g., Form A of Compound E, is substantially as shown in FIG. 17. In another embodiment, a solid form provided herein, e.g., Form A of Compound E, has one or more characteristic XRPD peaks at approximately 5.9702, 6.2798, 7.766, 11.9769, 12.4314, 14.8918, 15.5087, 16.002, 17.9217, 18.9264, 20.6365, 22.334, 23.8046, 25.8171, 26.1887±0.1° 2θ, as depicted in, for example, FIG. 17, and as found in Table 7 herein. In another embodiment, a solid form provided herein, e.g., Form A of Compound E, has at least 3, 5, 8, 10, or 12 characteristic XPRD peaks at approximately 5.9702, 6.2798, 7.766, 11.9769, 12.4314, 14.8918, 15.5087, 16.002, 17.9217, 18.9264, 20.6365, 22.334, 23.8046, 25.8171, 26.1887±0.1° 2θ, as depicted in, for example, FIG. 17, and as found in Table 7 herein. In still another embodiment, a solid form provided herein, e.g., Compound E, has at least 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, or all of the characteristic XPRD peaks at approximately 5.9702, 6.2798, 7.766, 11.9769, 12.4314, 14.8918, 15.5087, 16.002, 17.9217, 18.9264, 20.6365, 22.334, 23.8046, 25.8171, 26.1887±0.1° 2θ, as depicted in, for example, FIG. 17 and as found in Table 7 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound E, has at least 10 characteristic XPRD peaks at approximately 5.9702, 6.2798, 7.766, 11.9769, 12.4314, 14.8918, 15.5087, 16.002, 17.9217, 18.9264, 20.6365, 22.334, 23.8046, 25.8171, 26.1887±0.1° 2θ, as depicted in, for example, FIG. 17, and as found in Table 7 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound E, has at least 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 characteristic XPRD peaks at approximately 20.6365, 12.4314, 5.9702, 6.2798, 18.9264, 22.334, 14.8918, 25.8171, 16.002, 23.8046±0.1° 2θ, as depicted in, for example, FIG. 17, and as found in Table 7 herein.
In still another embodiment, a solid form provided herein, e.g., Form A of Compound E, has at least 5 characteristic XPRD peaks at approximately 5.9702, 6.2798, 7.766, 11.9769, 12.4314, 14.8918, 15.5087, 16.002, 17.9217, 18.9264, 20.6365, 22.334, 23.8046, 25.8171, 26.1887±0.1° 2θ, as depicted in, for example, FIG. 17, and as found in Table 7 herein. In still another embodiment, a solid form provided herein, e.g., Form A of Compound E, has at least 5 characteristic XPRD peaks at approximately 5.9702, 6.2798, 12.4314, 18.9264, 20.6365, 0.1° 2θ, as depicted in, for example, FIG. 17, and as found in Table 7 herein. In one embodiment, a solid form provided herein, e.g., Form A of Compound E, has an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 5.9702, 6.2798, 12.4314, 18.9264, 20.6365 (±0.1° 2θ).
TABLE 7
Representative XRPD Peaks for Compound E Form A
Pos. [º 2θ]
d-spacing [Å]
Rel. Int. [%]
5.9702
14.79172
72.39
6.2798
14.0631
69.41
7.766
11.37484
23.74
11.9769
7.38342
21.81
12.4314
7.11451
97.62
14.8918
5.94411
41.98
15.5087
5.70906
16.92
16.002
5.53413
36.61
17.9217
4.94544
23.26
18.9264
4.68511
63.17
20.6365
4.30057
100
22.334
3.97739
62.92
23.8046
3.73491
31.31
25.8171
3.44814
36.87
26.1887
3.40005
30.45
In another embodiment, Form A of Compound E is pure. In one such embodiment, Form A of Compound E is substantially free of other solid forms described herein (e.g. amorphous solid). In another embodiment, the purity of Form A of Compound E is no less than about 95%, no less than about 96%, no less than about 97%, no less than about 98%, no less than about 99%, no less than about 99.5%, or no less than about 99.9%.
Methods of Treating Cancer
The compounds and solid forms described herein can be administered to the patient in an effective amount (e.g. an amount as described herein) for treating cancer mediated by a KRasG12C mutation. In one such embodiment, the cancer is a solid tumor (e.g. lung cancer, CRC, or pancreatic cancer). It is to be understood that the methods described herein also include treatment with a pharmaceutical composition as described herein comprising a compound (e.g. Compound 1 or a solid form of Compound A, B, C, D, E, or F as described herein. In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a cancer, the method comprising administering an effective amount of a solid form corresponding to Compound A, B, C, D, E, or F, or a mixture thereof as described herein) to the patient having cancer.
In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound A as described herein to the patient. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of a solid form of Compound A (e.g. Form A, B, C, or D, or a mixture thereof) to the patient as described herein.
In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A as described herein. In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form A (e.g. substantially free of another solid form such as Compound A Form B, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form A is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form D as described herein. In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form D (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form C. In one such embodiment, the crystalline purity of Compound A Form D is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form C as described herein. In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form C (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form C is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form c comprising one or more solid form other than Form A Compound c. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C further comprising a percentage of Compound A Form A and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C comprising Compound A Form A and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form C includes Compound A Form A and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B as described herein. In one embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form B (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form B is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having lung cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B comprising one or more solid form other than Form A Compound B. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form B further comprising a percentage of Compound A Form A, Form C, and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form b comprising Compound A Form A, Form C, and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, 10%-50%, or 25%-75%. In another such embodiment, the mixture of Compound A Form B includes Compound A Form A, Form C and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound B as described herein to the patient. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of a solid form of Compound B (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound B Form A to the patient as described herein.
In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound C as described herein to the patient. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of a solid form of Compound C (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound C Form A to the patient as described herein.
In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound D as described herein to the patient. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of a solid form of Compound D (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound D Form A to the patient as described herein.
In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound E as described herein to the patient. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of a solid form of Compound E (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound E Form A to the patient as described herein.
In one embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound F as described herein to the patient. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of a solid form of Compound F (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating lung cancer mediated by a KRasG12C mutation in a patient having such a lung cancer, the method comprising administering an effective amount of Compound F Form A to the patient as described herein.
In such embodiments, the lung cancer is non-small cell lung cancer (NSCLC) comprising KRasG12C mutations. In another embodiment of the methods provided herein, the lung cancer is adenocarcinoma, squamous-cell lung carcinoma or large-cell lung carcinoma. In one such embodiment, the cancer is lung adenocarcinoma. In another such embodiment, the lung cancer is a small cell lung carcinoma. In another embodiment, the lung cancer is small cell lung carcinoma. In still another embodiment, the lung cancer is glandular tumors, carcinoid tumors or undifferentiated carcinomas. The lung cancer can be stage I or II lung cancer. In one embodiment, the lung cancer is stage 11 or IV lung cancer.
Further provided herein is the use (UL1) of Compound 1, Compound A, Compound B, Compound C, Compound D, Compound E, Compound F, or a solid form thereof as described herein for the treatment of lung cancer as described herein. Further provided herein is the use (UL2) of Compound A Form A as described herein for the treatment of lung cancer as described herein. Further provided herein is the use (UL3) of Compound A Form C as described herein for the treatment of lung cancer as described herein. Further provided herein is the use (UL4) of Compound A Form D as described herein for the treatment of lung cancer as described herein.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a cancer, the method comprising administering an effective amount of a solid form corresponding to Compound A, B, C, D, E, or F, or a mixture thereof as described herein) to the patient having cancer.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound A as described herein to the patient. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of a solid form of Compound A (e.g. Form A, B, C, or D, or a mixture thereof) to the patient as described herein.
In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A as described herein. In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form A (e.g. substantially free of another solid form such as Compound A Form B, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form A is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form D as described herein. In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form D (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form C. In one such embodiment, the crystalline purity of Compound A Form D is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form C as described herein. In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form C (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form C is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form c comprising one or more solid form other than Form A Compound c. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C further comprising a percentage of Compound A Form A and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C comprising Compound A Form A and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form C includes Compound A Form A and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B as described herein. In one embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form B (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form B is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having colorectal cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B comprising one or more solid form other than Form A Compound B. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form B further comprising a percentage of Compound A Form A, Form C, and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form b comprising Compound A Form A, Form C, and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, 10%-50%, or 25%-75%. In another such embodiment, the mixture of Compound A Form B includes Compound A Form A, Form C and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound B as described herein to the patient. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of a solid form of Compound B (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound B Form A to the patient as described herein.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound C as described herein to the patient. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of a solid form of Compound C (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound C Form A to the patient as described herein.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound D as described herein to the patient. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of a solid form of Compound D (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound D Form A to the patient as described herein.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound E as described herein to the patient. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of a solid form of Compound E (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound E Form A to the patient as described herein.
In one embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound F as described herein to the patient. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of a solid form of Compound F (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating colorectal cancer mediated by a KRasG12C mutation in a patient having such a colorectal cancer, the method comprising administering an effective amount of Compound F Form A to the patient as described herein.
Further provided herein is the use (UC1) of Compound 1, Compound A, Compound B, Compound C, Compound D, Compound E, Compound F, or a solid form thereof as described herein for the treatment of colorectal cancer as described herein. Further provided herein is the use (UC2) of Compound A Form A as described herein for the treatment of colorectal cancer as described herein. Further provided herein is the use (UC3) of Compound A Form C as described herein for the treatment of colorectal cancer as described herein. Further provided herein is the use (UC4) of Compound A Form D as described herein for the treatment of colorectal cancer as described herein.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a cancer, the method comprising administering an effective amount of a solid form corresponding to Compound A, B, C, D, E, or F, or a mixture thereof as described herein) to the patient having cancer.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound A as described herein to the patient. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of a solid form of Compound A (e.g. Form A, B, C, or D, or a mixture thereof) to the patient as described herein.
In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A as described herein. In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form A (e.g. substantially free of another solid form such as Compound A Form B, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form A is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form D as described herein. In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form D (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form C. In one such embodiment, the crystalline purity of Compound A Form D is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form C as described herein. In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form C (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form C is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form c comprising one or more solid form other than Form A Compound c. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C further comprising a percentage of Compound A Form A and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C comprising Compound A Form A and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form C includes Compound A Form A and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B as described herein. In one embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form B (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form B is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having pancreatic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B comprising one or more solid form other than Form A Compound B. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form B further comprising a percentage of Compound A Form A, Form C, and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form b comprising Compound A Form A, Form C, and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, 10%-50%, or 25%-75%. In another such embodiment, the mixture of Compound A Form B includes Compound A Form A, Form C and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound B as described herein to the patient. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of a solid form of Compound B (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound B Form A to the patient as described herein.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound C as described herein to the patient. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of a solid form of Compound C (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound C Form A to the patient as described herein.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound D as described herein to the patient. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of a solid form of Compound D (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound D Form A to the patient as described herein.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound E as described herein to the patient. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of a solid form of Compound E (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound E Form A to the patient as described herein.
In one embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound F as described herein to the patient. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of a solid form of Compound F (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating pancreatic cancer mediated by a KRasG12C mutation in a patient having such a pancreatic cancer, the method comprising administering an effective amount of Compound F Form A to the patient as described herein.
Further provided herein are methods of treating tumor agnostic cancer comprising a KRasG12C mutation in a patient having such a cancer. In one such embodiment, the method comprising treating tumor agnostic cancer comprising a KRasG12C mutation in a patient having such a cancer by
(a) determining the absence or presence of a KRasG12C mutation in a sample taken from a patient with a suspected diagnosed cancer; and
(b) administering to the patient an effective amount of a solid form of Compound A (e.g. Form A, B, C, or D, or a mixture thereof) to the patient as described herein.
In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A as described herein. In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form A (e.g. substantially free of another solid form such as Compound A Form B, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form A is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form D as described herein. In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form D (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form C. In one such embodiment, the crystalline purity of Compound A Form D is 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form A comprising one or more solid form other than Form A Compound A. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form D may include Compound A Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%. In another such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A further comprising a percentage of Compound A Form C. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form A comprising Compound A Form C at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form A and Form C may include Compound A Form C at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form C as described herein. In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form C (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form B, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form C is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form c comprising one or more solid form other than Form A Compound c. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C further comprising a percentage of Compound A Form A and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form C comprising Compound A Form A and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, or 10%-50%. In another such embodiment, the mixture of Compound A Form C includes Compound A Form A and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B as described herein. In one embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of pure Compound A Form B (e.g. substantially free of another solid form such as Compound A Form A, Compound A Form C, or Compound A Form D. In one such embodiment, the crystalline purity of Compound A Form B is 80%, 85%, 90%, 95%, 97%, 98%, 98.5%, 99%, 99.5%, 99.9%. In another embodiment, the method comprises administering to the patient having a tumor agnostic cancer comprising a KRasG12C mutation, an effective amount of Compound A Form B comprising one or more solid form other than Form A Compound B. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form B further comprising a percentage of Compound A Form A, Form C, and/or Form D. In one such embodiment, the method comprises administering to the patient an effective amount of Compound A Form b comprising Compound A Form A, Form C, and/or Form D at a percentage of about 0.1%-10%, 0.5%-20%, 1%-30%, 1%-40%, 1%-50%, 10%-50%, or 25%-75%. In another such embodiment, the mixture of Compound A Form B includes Compound A Form A, Form C and/or Form D at an amount of less than about 0.5%, 1%, 2%, 5%, 7%, 10%, 15%, 20%, 25%, 40%, 50%, 60%, 75%, 80%, or 90%.
In one embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound B as described herein to the patient. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of a solid form of Compound B (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound B Form A to the patient as described herein.
In one embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound C as described herein to the patient. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of a solid form of Compound C (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound C Form A to the patient as described herein.
In one embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound D as described herein to the patient. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of a solid form of Compound D (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound D Form A to the patient as described herein.
In one embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound E as described herein to the patient. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of a solid form of Compound E (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound E Form A to the patient as described herein.
In one embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound F as described herein to the patient. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of a solid form of Compound F (e.g. Form A) to the patient as described herein. In one such embodiment is a method of treating a tumor agnostic cancer mediated by a KRasG12C mutation in a patient having such a tumor agnostic cancer, the method comprising administering an effective amount of Compound F Form A to the patient as described herein.
Further provided herein is the use (UP1) of Compound 1, Compound A, Compound B, Compound C, Compound D, Compound E, Compound F, or a solid form thereof as described herein for the treatment of tumor agnostic cancer as described herein. Further provided herein is the use (UP2) of Compound A Form A as described herein for the treatment of tumor agnostic cancer as described herein. Further provided herein is the use (UP3) of Compound A Form C as described herein for the treatment of tumor agnostic cancer as described herein. Further provided herein is the use (UP4) of Compound A Form D as described herein for the treatment of tumor agnostic cancer as described herein.
In one embodiment of the methods and uses described herein, Compound 1 or a solid form described herein (e.g. Compound A Form A/B/C/D, Compound B, Compound C, Compound D, Compound E, or Compound F) is administered as a fixed dose QD administration. In one embodiment, the administration is oral (PO), where Compound 1 or a solid form described herein (e.g. Compound A Form A/B/C/D, Compound B, Compound C, Compound D, Compound E, or Compound F) is formulated as a tablet or capsule. In one embodiment, Compound 1 or a solid form described herein (e.g. Compound A Form A/B/C/D, Compound B, Compound C, Compound D, Compound E, or Compound F) is administered at an amount of 5 mg-600 mg, 5 mg-500 mg, 5 mg-400 mg, 5 mg-300 mg, 5 mg-250 mg, 5 mg-200 mg, 5 mg-150 mg, 5 mg-100 mg, 5 mg-50 mg, 5 mg-25 mg, 25 mg-600 mg, 25 mg-500 mg, 25 mg-400 mg, 25 mg-300 mg, 25 mg-250 mg, 25 mg-200 mg, 25 mg-150 mg, 25 mg-100 mg, 25 mg-50 mg, 50 mg-600 mg, 50 mg-500 mg, 50 mg-400 mg, 50 mg-300 mg, 50 mg-250 mg, 50 mg-200 mg, 50 mg-150 mg, or 50 mg-100 mg QD. In another embodiment, Compound 1 or a solid form described herein (e.g. Compound A Form A/B/C/D, Compound B, Compound C, Compound D, Compound E, or Compound F) is administered at an amount of about 5 mg, 25 mg, 50 mg, 100 mg, 150 mg, 200 mg, 250 mg, 300 mg, 400 mg or 500 mg. In another embodiment, Compound A Form A or Compound A Form D as described herein is administered at an amount of about 5 mg, 25 mg, 50 mg, 100 mg, 150 mg, 200 mg, 250 mg, 300 mg, 400 mg or 500 mg.
Kits:
Compound 1 and the solid forms described herein (e.g. Compound A, Compound B, Compound C, Compound D, Compound E, and/or Compound F) can be provided as an article of manufacture (i.e a kit) comprising one or more of the compounds described herein for administration. In one embodiment, the kit includes Compound A or a solid form thereof as described herein (e.g. Compound A Form A, B, C, or D) for administration as described herein. In one such embodiment, a kit as described herein comprises Compound A Form A or Compound A Form D as described herein. In another embodiment, the kit includes Compound B Form A. In another embodiment, the kit includes Compound C Form A. In still another embodiment, the kit includes Compound D Form A. In still another embodiment, the kit includes Compound E form A. In still another embodiment, the kit includes Compound F Form A.
In some instances, the article of manufacture further comprises package insert comprising instructions to treat or delay progression of a solid tumor (e.g. lung cancer, CRC, or pancreatic cancer as described herein). In one such embodiment, the cancer is NSCLC. In one embodiment, the article of manufacture further comprises package insert comprising instructions for using Compound 1 or solid forms described herein (e.g. Compound A, Compound B, Compound C, Compound D, Compound E, and/or Compound F) to treat or delay progression of NSCLC in a patient. In one embodiment, the article of manufacture further comprises package insert comprising instructions for using Compound 1 or a solid forms described herein (e.g. Compound A, Compound B, Compound C, Compound D, Compound E, and/or Compound F) to treat or delay progression of pancreatic cancer in a patient. In one embodiment, the article of manufacture further comprises package insert comprising instructions for using Compound 1 or a solid forms described herein (e.g. Compound A, Compound B, Compound C, Compound D, Compound E, and/or Compound F) to treat or delay progression of CRC in a patient.
In such kits, Compound 1 or a solid forms described herein (e.g. Compound A, Compound B, Compound C, Compound D, Compound E, and/or Compound F) is provided in a container. Suitable containers include, for example, bottles, vials, bags and syringes. The container may be formed from a variety of materials such as glass, plastic (such as polyvinyl chloride or polyolefin), or metal alloy (such as stainless steel or hastelloy). In some instances, the container holds the formulation and the label on, or associated with, the container may indicate directions for use. The article of manufacture or kit may further include other materials desirable from a commercial and user standpoint, including other buffers, diluents, filters, needles, syringes, and package inserts with instructions for use. In some instances, the article of manufacture further includes one or more of another agent (e.g., an additional chemotherapeutic agent or anti-neoplastic agent). Suitable containers for the one or more agents include, for example, bottles, vials, bags and syringes.
Any of the articles of manufacture or kits described herein may include instructions to administer Compound 1 or a solid form described herein (e.g. Compound A, Compound B, Compound C, Compound D, Compound E, and/or Compound F) to a patient in accordance with any of the methods described herein.
Embodiments
Provided below are some exemplary embodiments of the invention.
Embodiment 1. A compound having the structure:
Embodiment 2. A crystal form comprising Compound A
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 9.6474, 11.0365, 15.4059, 16.4193, 18.7038 (±0.1° 2θ).
Embodiment 3. The crystal form of embodiment 2, wherein the crystal form of Compound A has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 1.
Embodiment 4. The crystal form of embodiment 2, wherein the crystal form of Compound A has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 1.
Embodiment 5. The crystal form of embodiment 2, wherein the crystal form of Compound A has an X-ray powder diffraction pattern substantially as shown in FIG. 1.
Embodiment 6. The crystal form of embodiment 2, wherein the crystal form of Compound A has a TGA thermograph corresponding substantially to the representative TGA thermogram as depicted in FIG. 2.
Embodiment 7. The crystal form of embodiment 2, wherein the crystal form of Compound A has a DSC thermograph corresponding substantially as depicted in FIG. 2.
Embodiment 8. A crystal form comprising Compound A:
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 5.2063, 14.63, 17.7161, 21.9253, 25.1335 (±0.1° 2θ).
Embodiment 9. The crystal form of embodiment 8, wherein the crystal form of Compound A has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 2.
Embodiment 10. The crystal form of embodiment 8, wherein the crystal form of Compound A has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 2.
Embodiment 11. The crystal form of embodiment 8, wherein the crystal form of Compound A has an X-ray powder diffraction pattern substantially as shown in FIG. 5.
Embodiment 12. A crystal form comprising Compound A:
Embodiment 13. A crystal form comprising Compound A:
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 9.7745, 11.0487, 15.2452, 18.6477, 18.7908 (±0.1° 2θ).
Embodiment 14. The crystal form of embodiment 13, wherein the crystal form of Compound A has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 3.
Embodiment 15. The crystal form of embodiment 13, wherein the crystal form of Compound A has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 3.
Embodiment 16. The crystal form of embodiment 13, wherein the crystal form of Compound A has an X-ray powder diffraction pattern substantially as shown in FIG. 8.
Embodiment 17. The crystal form of embodiment 13, wherein the crystal form of Compound A has a TGA thermograph corresponding substantially to the representative TGA thermogram as depicted in FIG. 10.
Embodiment 18. The crystal form of embodiment 13, wherein the crystal form of Compound A has a DSC thermograph corresponding substantially as depicted in FIG. 9.
Embodiment 19. A crystal form comprising Compound B:
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 6.6796, 14.9097, 15.2963, 19.4416, 23.7124 (±0.1° 2θ).
Embodiment 20. The crystal form of embodiment 19, wherein the crystal form of Compound B has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 4.
Embodiment 21. The crystal form of embodiment 19, wherein the crystal form of Compound B has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 4.
Embodiment 22. The crystal form of embodiment 19, wherein the crystal form of Compound B has an X-ray powder diffraction pattern substantially as shown in FIG. 11.
Embodiment 23. The crystal form of embodiment 19, wherein the crystal form of Compound B has a DSC thermograph corresponding substantially as depicted in FIG. 12.
Embodiment 24. A crystal form comprising Compound C:
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 12.5401, 17.5707, 16.834, 21.3525, 26.5569 (±0.1° 2θ).
Embodiment 25. The crystal form of embodiment 24, wherein the crystal form of Compound C has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 5.
Embodiment 26. The crystal form of embodiment 24, wherein the crystal form of Compound C has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 5.
Embodiment 27. The crystal form of embodiment 24, wherein the crystal form of Compound C has an X-ray powder diffraction pattern substantially as shown in FIG. 13.
Embodiment 28. The crystal form of embodiment 24, wherein the crystal form of Compound C has a TGA thermograph corresponding substantially to the representative TGA thermogram as depicted in FIG. 14.
Embodiment 29. The crystal form of embodiment 24, wherein the crystal form of Compound C has a DSC thermograph corresponding substantially as depicted in FIG. 14.
Embodiment 30. A crystal form comprising Compound D:
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 7.3809, 10.7407, 14.654, 18.5979, 25.2558 (±0.1° 2θ).
Embodiment 31. The crystal form of embodiment 30, wherein the crystal form of Compound D has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 6.
Embodiment 32. The crystal form of embodiment 30, wherein the crystal form of Compound D has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 6.
Embodiment 33. The crystal form of embodiment 30, wherein the crystal form of Compound D has an X-ray powder diffraction pattern substantially as shown in FIG. 15.
Embodiment 34. The crystal form of embodiment 30, wherein the crystal form of Compound D has a TGA thermograph corresponding substantially to the representative TGA thermogram as depicted in FIG. 16.
Embodiment 35. The crystal form of embodiment 30, wherein the crystal form of Compound D has a DSC thermograph corresponding substantially as depicted in FIG. 16.
Embodiment 36. A crystal form comprising Compound E:
having an X-ray powder diffraction pattern comprising characteristic X-ray powder diffraction peaks using CuKα radiation at 5.9702, 6.2798, 12.4314, 18.9264, 20.6365 (±0.1° 2θ).
Embodiment 37. The crystal form of embodiment 36, wherein the crystal form of Compound E has an X-ray powder diffraction pattern comprising at least 5 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 7.
Embodiment 38. The crystal form of embodiment 36, wherein the crystal form of Compound E has an X-ray powder diffraction pattern comprising at least 10 characteristic X-ray powder diffraction peaks using CuKα radiation as set forth in Table 7.
Embodiment 39. The crystal form of embodiment 36, wherein the crystal form of Compound E has an X-ray powder diffraction pattern substantially as shown in FIG. 17.
Embodiment 40. A pharmaceutical composition comprising the solid form of any one of claims 2-39 and at least one pharmaceutically acceptable excipient.
Embodiment 41. A pharmaceutical composition of embodiment 40, wherein said composition is formulated for oral administration.
Embodiment 42. A method of treating a cancer comprising a KRasG12C mutation in a patient having said cancer, the method comprising administering an effective amount of a compound of embodiment 1 or a crystal form of any one of embodiments 2-39.
Embodiment 43. A method for treating a cancer comprising a KRasG12C mutation in a patient having said cancer, the method comprising:
determining if the patient has the mutation; and
if the patient is determined to have the mutation, then administering to the patient an effective amount of a compound of claim 1 or a crystal form of any one of embodiments 2-39.
Embodiment 44. The method of embodiment 42 or 43, wherein the cancer comprises lung cancer, colorectal cancer, or pancreatic cancer.
Embodiment 45. The method of embodiment 42 or 43, wherein the cancer is lung cancer.
Embodiment 46. The method of embodiment 45, wherein the lung cancer is non-small cell lung cancer (NSCLC).
Embodiment 47. The method of embodiment 42 or 43, wherein the cancer is colorectal cancer.
Embodiment 48. The method of embodiment 42 or 43, wherein the cancer is pancreatic cancer.
Embodiment 49. A method for inhibiting proliferation of a cell population wherein the cell population comprises a KRasG12C mutation, the method comprising contacting the cell population with a compound of claim 1 or a crystal form of any one of embodiments 2-39.
Embodiment 50. A method for inhibiting tumor metastasis comprising administering to an individual in need thereof a therapeutically effective amount of the compound of embodiment 1 or a crystal form of any one of embodiments 2-39.
Embodiment 51. Use of a compound of embodiment 1 or a crystal form of any one of embodiments 2-39 in the manufacture of a medicament for treating a cancer.
Embodiment 52. The use of embodiment 51, wherein the cancer comprises lung cancer, colorectal cancer, or pancreatic cancer.
Embodiment 53. The compound of claim 1 or a crystal form of any one of embodiments 2-39 for use in a method of treating cancer.
Embodiment 54. The compound of embodiment 53, wherein the cancer comprises lung cancer, colorectal cancer, or pancreatic cancer.
EXAMPLES
The following Examples are presented by way of illustration, not limitation.
Example 1
Compound 1 was initially screened with 21 acids and four solvent systems for pharmaceutically acceptable salts and polymorphs. (Table 8). For each solvent of acetone, EtOAc, THF, and MeOH/H2O (19:1, v/v), freebase and corresponding acid were mixed with a molar charge ratio of 1:1, and stirred at RT overnight. Due to the observation that all the samples were clear solution, all the samples were transferred to stirring at 5° C. overnight. The solids obtained at 5° C. were tested by XRPD. For the clear solutions, anti-solvent (n-heptane for acetone, THF and EtOAc; H2O for MeOH/H2O) was added. The mixtures were then stirred at 5° C. for 3 days. The solids obtained were characterized by XRPD, and the other samples were transferred to heating-cooling between 5-50° C. The solids obtained were characterized by XRPD, and the clear solutions were transferred to slow evaporation at RT.
TABLE 8
MeOH/H2O
Solvent
Acetone
THF
EtOAc
(19:1, v/v)
Blank
Freebase Form
Freebase Form A
Amorphous$
Gel$
A$
(Low crystallinity)$
H3PO4
Amorphous$
Amorphous*
Amorphous*
Gel$
Acetic acid
Compound E
Compound E
Amorphous$
Gel$
Form A$
Form A$
Maleic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
Fumaric acid&&
Compound B
Low crystallinity*
Low crystallinity&
Gel$
Form A**
Compound B
Low crystallinity*
Low crystallinity&
Gel (EtOH)
Form A&
Succinic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
L-Malic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
Adipic acid
Compound A
Compound A
Adipate Type A&
Gel$
Form A&
Form A*
L-Tartaric acid
Amorphous$
Amorphous*
Acid*
Gel$
Hippuric acid
Amorphous$
Amorphous$
Amorphous$
Gel$
Citric acid
Amorphous$
Amorphous*
Acid**
Gel$
Glycolic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
Malonic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
Benzoic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
Gentisic acid
Amorphous$
Amorphous$
Amorphous*
Gel$
Oxalic acid
Amorphous$
Amorphous$
Amorphous**
Gel$
R-mandelic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
S-mandelic acid
Amorphous$
Amorphous$
Amorphous$
Gel$
p-Toluensulfonic
Gel$
Amorphous$
Amorphous$
Gel$
acid
Benzenesulfonic
Compound D
Amorphous$
Amorphous$
Gel$
acid
Form A$
Methylsulfonic
Compound E
Amorphous&
Amorphous$
Gel$
acid
Form A#
Ethylsulfonic acid
Amorphous$
Amorphous$
Compound C
Gel$
Form A&
&: Obtained from slurry at 5° C.
*: Anti-solvent of n-heptane was added and stirred at 5° C.
**: Anti-solvent of n-heptane was added and stirred at 5° C. Heating-cooling between 5° C. and 50° C. was performed.
#: Limited solids were observed after stirring at 5° C. During XRPD test, it was observed that the sample may tend to absorb moisture and turn to liquid. The suspension was transferred to −20° C., but limited solids were still observed. Anti-solvent (n-heptane) was added and the sample was transferred to 5° C. However, gel was obtained.
$: Anti-solvent was added and stirred at 5° C. Heating-cooling between 5° C. and 50° C. was performed, followed by slow evaporation at RT.
&&: For fumaric acid, to try to obtain potential anhydrous/hydrous fumarate hits with good crystallinity, experiments in acetone, THF, and EtOAc were repeated, and one more experiment in EtOH was also set up. However, anhydrous/hydrous fumarate hit with better crystallinity was not obtained.
As summarized in Table 9, a total of six crystalline hits were obtained. The salt hits were characterized by XRPD, TGA, DSC, HPLC and NMR.
TABLE 9
Characterization summary of crystalline salt hits
Weight
Endotherm in
Purity
Stoich-
Loss in
DSC (° C.,
iometry
Salt
TGA (%)
peak)
(area %)
(acid/base)
Compound A Form A
2.0
68.8, 169.1
98.30
1.06
Compound B Form A
0.7
53.8, 156.3
93.56
1.03
Compound C Form A
8.6
81.0, 149.2
95.18
1.04
Compound D Form A
7.7
75.8
96.23
1.03
Compound E Form A
NA
NA
NA
NA
Compound F Form A
9.0
65.5, 125.4
88.42
0.69
A diverse range of conditions was also explored by carrying out maturation at two different temperatures starting with the amorphous material from a diverse range of solvent/solvent mixtures.
Amorphous material (25 mg) in HPLC vials was treated with 5 vol (125 μl) of solvent and the samples were placed on a shaker at 50° C. or on a stirrer at 5° C. for 7 days with observations noted upon solvent addition. Any solids were filtered using a fritted filter and initially analysed by XRPD. Any solutions were treated with anti-solvent in increasing solvent:anti-solvent ratios until a maximum ratio of 1:5 had been reached at 25° C. The samples were then cooled to 5° C. at 0.1° C./min and held over the weekend. Any solutions from cooling were left to evaporate at RT with the caps removed and any turbid samples were filtered using a fritted filter and initially analysed by XRPD.
Maturation at both low and high temperature for 7 days starting with the amorphous material resulted in the majority of samples remaining as solutions. The solutions from 50° C. maturation were treated with anti-solvent which largely remained as clear solutions after addition of 1:5 solvent:anti-solvent ratio and cooling to 5° C. The samples were subsequently evaporated which largely resulted in amorphous, Compound A Form A/D or gums. The solutions obtained from 5° C. maturation were kept at 5° C. for the duration of the project and remained as solutions.
TABLE 10
Results and observations from maturation at 5° C. for 7 days starting
on amorphous.
Solvent
Upon addition at 5° C.
After 5° C. maturation
XRPD
Water
Clear Solution
Clear Solution
N/P
Methanol
Clear Solution
Clear Solution
N/P
Ethanol
Clear Solution
Clear Solution
N/P
2-propanol
Clear Solution
Suspension
Insufficient
material
1-propanol
Clear Solution
Clear Solution
N/P
Acetone
Clear Solution
Clear Solution
N/P
Ethyl Acetate
Clear Solution
Suspension
Insufficient
material
Acetonitrile
Clear Solution
Turbid
Insufficient
material
Toluene
Clear Solution
Solution + fine particles
N/P
Isopropyl Acetate
Clear Solution
Solution + fine particles
N/P
TBME
Turbid/ Hazy
Hazy Solution
N/P
2-butanone (MEK)
Clear Solution
Clear Solution
N/P
THF
Clear Solution
Clear Solution
N/P
DMSO
Clear Solution
Clear Solution
N/P
NMP
Clear Solution
Clear Solution
N/P
Diethyl ether
Hazy Solution
Turbid/ Hazy
Amorphous
MIBK
Clear Solution
Turbid/Hazy
Insufficient
material
DCM
Clear Solution
Clear Solution
N/P
Xylene
Partially Dissolved
Solution + large particles
N/P
DMI
Clear Solution
Clear Solution
N/P
Cumene
Partially Dissolved
Solution + large particles
N/P
Sulfolane
Clear Solution
Clear Solution
N/P
DMPU
Clear Solution
Clear Solution
N/P
2-Methyl THF
Clear Solution
Clear Solution
N/P
Heptane
Turbid/Hazy
Hazy Solution
N/P
1,4-dioxane
Clear Solution
Clear Solution
N/P
DMF
Clear Solution
Clear Solution
N/P
Nitromethane
Clear Solution
Solution + fine particles
N/P
Chloroform
Clear Solution
Clear Solution
N/P
1-butanol
Clear Solution
Clear Solution
N/P
1-Methoxy-2-propanol
Clear Solution
Clear Solution
N/P
3-Methyl-1-butanol
Clear Solution
Clear Solution
N/P
Anisole
Clear Solution
Clear Solution
N/P
t-butanol/water (1:1)
Clear Solution
Clear Solution
N/P
Solvent
Upon addition at 5° C.
After 5° C. maturation
XRPD
10% water/ methanol
Clear Solution
Clear Solution
N/P
5% water/EtOH
Clear Solution
Clear Solution
N/P
20% water/ methanol
Clear Solution
Clear Solution
N/P
10% water/EtOH
Clear Solution
Clear Solution
N/P
10% water/IPA
Clear Solution
Clear Solution
N/P
10% water/ACN
Clear Solution
Clear Solution
N/P
10% water/Acetone
Clear Solution
Clear Solution
N/P
PEG 400
Clear Solution
Clear Solution
N/P
Tetralin
Partially Dissolved
Gummy Solution
N/P
Cyclohexane
Thin Suspension
Very Thin Suspension
Amorphous
Acetic Acid
Clear Solution
Clear Solution
N/P
Hexane
Thin Suspension
Turbid
Insufficient
material
Ethyleneglycol
Clear Solution
Clear Solution
N/P
Pyridine
Clear Solution
Clear Solution
N/P
TABLE 11
Results and observations from anti-solvent addition from 50 ° C.
maturation
Antisolvent
added at RT
(solvent:anti-
solvent ratio)
Upon cooling
Solvent
Antisolvent
1:1
1:3
1:5
to 5° C.
XRPD
Water
3-Methyl-1-
✓
+/−
+/−
Cloudy Solution
Very little solid, poor
butanol
signal, Form A/D
Methanol
Xylene
✓
✓
✓
Frozen
Gummy, amorphous
Ethanol
Diethyl ether
✓
✓
✓
Clear Solution
Gummy, very poor
signal, Form A/D
2-propanol
Diethyl ether
✓
✓
✓
Clear Solution
Gummy
1-propanol
Diethyl ether
✓
✓
✓
Clear Solution
Gummy, partial match
Form A/D, extra peaks
Acetone
Diethyl ether
✓
✓
✓
Cloudy Solution
Very Poorly Crystalline
2-butanone
Diethyl ether
✓
✓
✓
Clear Solution
Form A/D
(MEK)
THF
Diethyl ether
✓
✓
✓
Clear Solution
Form A/D
DMSO
Ethyl
✓
✓
✓
Clear Solution
Amorphous
Acetate
NMP
Ethyl
✓
✓
✓
Clear Solution
Amorphous
Acetate
DCM
Ethyl
X
Turbid/Hazy
Poorly Crystalline,
Acetate
Form A/D
DMI
Ethyl
✓
✓
+/−
Clear Solution
Amorphous
Acetate
Sulfolane
Ethyl
✓
✓
✓
Clear Solution
Clear Solution - after
Acetate
vac drying
DMPU
Ethyl
✓
✓
✓
Clear Solution
Amorphous
Acetate
2-Methyl THF
Diethyl ether
✓
+/−
+/−
Partially Cloudy
Form A/D
Solution
1,4-dioxane
Diethyl ether
X
Gummy solution
Very little solid,
insufficient material
DMF
Diethyl ether
✓
✓
✓
Clear Solution
Very little solid,
insufficient material
Nitromethane
Diethyl ether
✓
✓
+/−
Gummy solution
Gummy, poor signal,
Form A/D
Chloroform
Diethyl ether
X
Turbid
Poorly Crystalline,
Form A/D
1-butanol
Diethyl ether
✓
✓
✓
Clear Solution
Gummy, amorphous
1-Methoxy-2-
IPA
✓
✓
✓
Clear Solution
Gummy
propanol
3-Methyl-1-
IPA
✓
✓
✓
Clear Solution
Gummy
butanol
t-butanol/water
IPA
✓
✓
✓
Clear Solution
Gummy
(1:1)
10%
IPA
✓
✓
✓
Clear Solution
Gummy
water/methanol
5% water/EtOH
Xylene
✓
✓
✓
Frozen
Form A/D
20%
IPA
✓
✓
✓
Clear Solution
Very little solid,
water/methanol
insufficient material
10%
Xylene
✓
+/−
+/−
Frozen
Very little solid,
water/EtOH
amorphous
10% water/IPA
Xylene
✓
✓
✓
Frozen
Very Poorly Crystalline
10% water/ACN
Xylene
✓
✓
✓
Frozen
Gummy, amorphous
10%
Xylene
✓
✓
✓
Partially Frozen
Oily Residue
water/Acetone
PEG 400
Diethyl ether
✓
+/−
+/−
Biphasic Layers
Clear gel like solution
Acetic Acid
Diethyl ether
✓
✓
✓
Clear Solution
Very little solid,
insufficient material
Ethyleneglycol
Diethyl ether
✓
✓
✓
Clear Solution
Amorphous
Pyridine
Diethyl ether
✓
✓
✓
Clear Solution
Gummy, amorphous
Example 2
A total of 62 polymorph screening experiments were performed for freebase through different crystallization methods. Compared with the starting material, better crystallinity was observed for the sample obtained by slow evaporation in ACN with adipic acid, and named as Compound A Form A.
Single crystal data of Compound A Form A was obtained as shown in FIG. 4. According to the single crystal analysis result, Compound A Form A is anhydrous in the lattice, but might contain some surface water.
Compound A Form A was prepared by slurry freebase and adipic acid in EtOAc at RT for 48 hrs and then transferred to 5° C. for 24 hrs to increase the yield. The wet sample was vacuum dried at RT for 3 hrs. No form change was observed before and after drying. A solid was obtained with a yield of 62.2%. As per TGA and DSC, the sample showed a weight loss of 0.6% up to 100° C., and DSC curve showed two endotherms at 56.0° C. and 168.7° C. (peak temperature). Based on the integrals in NMR spectrum, the stoichiometric ratio of adipic acid:freebase was determined to be 1.06. A peak of EtOAc was observed. Around 0.07 molar EtOAc (0.8 wt %) was detected, which was consistent with TGA weight loss.
A disordered version of Compound A Form A, designated as Compound A Form C, was identified via single crystal XRD. See FIG. 7. Further description of this form and its interchangeability with Compound A Form A and Compound A Form D is below.
Compound A Form A was exposed to ambient humidity levels 40%, whereupon Compound A Form D was formed. Compound A Form D is a hemihydrate form of Compound A. For reversibility, Compound A Form D was dehydrated, whereupon Compound A Form D formed Compound A Form C.
Another form of Compound A was obtained and designated as Form B. Compound A Form B was obtained from anti-solvent addition in DCM/toluene, followed by transferring to 5° C. No form change was observed after air drying at RT overnight. A weight loss of 2.2% up to 100° C. was observed in TGA, and two broad endotherms at 55.7° C. and 109.6° C. (peak), and one small endotherm at 158.8° C. (peak) were observed in DSC. Based on the integrals, the stoichiometric ratio of adipic acid:freebase was determined to be 1.65.
VT-XRPD was performed on Compound A Form B for form identification. After heating to 90° C. under N2 protection, no form change was observed, indicating the TGA weight loss was caused by surface water. Thus, Compound A Form B was speculated to be an anhydrate. No peak of DCM was observed. To further confirm the stoichiometric ratio, three batches of Compound A Form B were re-prepared by anti-solvent addition in DCM/toluene, followed by transferring to 5° C. Based on the NMR results, the stoichiometric ratio of adipic acid:freebase for Compound A Form B varied from 1.5 to 1.8.
Slurry Competition between Compound A Form A and B. Slurry competition experiments between Compound A Form A and B were set up to determine the relationship between these two anhydrates. The saturated solution of Compound A Form A was obtained via slurry of Compound A Form A at target temperature overnight. A mixture of Compound A Form A+B was added into ˜0.7 mL of saturated solution of Compound A Form A, and suspensions were observed. The suspensions were stirred at a speed of 750 rpm and tested by XRPD in transmission mode. As summarized in Table 12, in toluene, after a mixture of Compound A Form A+B was stirred at 5° C., a mixture of Compound A Form A+B was observed after 5 days. After transferring the sample to RT, Compound A Form A was observed after slurry at RT for 18 days (the peak at ˜18.1° was possibly caused by stirrer). In IPA, the mixture turned to Compound A Form A at both 5° C. and −20° C.
TABLE 12
Slurry competition between adipate Type A and B
Starting Form
Temperature (° C.)
Solvent
Result
Compound A Form
5 to RT
Toluene
Compound A Form A
A + B
5
IPA
Compound A Form A
−20
IPA
Compound A Form A
Two adipate forms of anhydrates Compound A Form A and Compound A Form B were observed from polymorph screening of adipate with Compound 1. It should be noted that although Compound A Form A was a mono-salt, the stoichiometry of acid/freebase for different Compound A Form B batches varied from 1.5 to 2.1, suggesting Compound A Form B might be a sesqui- or bis-salt. Slurry competition experiments between Compound A Form A and B in toluene (RT) and IPA (5° C. and −20° C.) resulted in Compound A Form A.
Reactive Crystallisation with Adipic Acid. Additional steps were investigated to identify whether additional forms of the adipate salt exist when starting from the free form of Compound 1.
Compound 1 (30 mg) was weighed into HPLC vials with stirrers and dissolved at 50° C. Adipic acid solution in THF (1 M, 1 or 1.5 eq.) was added to each vial and if a solid formed, then an aliquot was taken. The solutions or suspensions were cooled to 40° C. at 0.5° C./min when they were seeded with a very small amount of Compound A Form A. The samples were then further cooled to 5° C. at 0.1° C./min overnight and if a precipitate formed, it was filtered and analysed by XRPD.
Reactive crystallisation with adipic acid largely resulted in Compound A Form A/D or sticky material which was amorphous by XRPD. The results and observations from reactive crystallisation with adipic acid are summarised below in Table 13.
TABLE 13
Solvent
Obs. After acid
Obs. After cooling
Solvent
Acid
vol.
addition
to 5° C.
XRPD
Water
1
40*
Became clear
Clear Solution
N/P
10%
equivalent
30
Clear Solution
Clear Solution
Sticky material,
water/IPA
adipic
amorphous
EtOH
acid
20
Clear Solution
Clear Solution
Form A/D
Ethyl
30
Light Precipitate
White Precipitate
Form A/D
acetate
Acetone
20
Clear Solution
Clear Solution
Form A/D
Acetonitrile
30
Clear Solution
White Precipitate
Form A/D
MEK
20
Clear Solution
Clear Solution
Form A/D
THF
5
Clear Solution
White Precipitate, fine
Form A/D
TBME
40*
White Precipitate
White Precipitate
Form A/D (both & A)
Dioxane
10
Clear Solution
Clear Solution
Sticky material,
amorphous
Anisole
20
Gel-like suspen-
White Precipitate
Form A/D (both & A)
sion at 40° C.
Acetic acid
5
Clear Solution
Clear Solution
Sticky material, N/P
Water
1.5
40*
Partially Clear
Clear Solution
N/P
10%
equivalents
30
Clear Solution
Clear Solution
Sticky material,
water/IPA
adipic
amorphous
EtOH
acid
20
Clear Solution
Clear Solution
Form A/D
Ethyl
30
White Precipitate,
White Precipitate
Form A/D (both & A)
acetate
at 40° C.
Acetone
20
Clear Solution
Clear Solution
Form A/D
Acetonitrile
30
Clear Solution
White Precipitate
Form A/D
MEK
20
Clear Solution
White Precipitate
Form A/D
THF
5
Clear Solution
White Precipitate,
Form A/D
fine
TBME
40*
White Precipitate
White Precipitate
Form A/D (both & A)
Dioxane
10
Clear Solution
Clear Solution
Sticky material,
amorphous
Anisole
20
Gel-like suspen-
White Precipitate
Form A/D (both & A)
sion at 40° C.
Acetic acid
5
Clear Solution
Clear Solution
Sticky material,
amorphous
Example 3
Instruments and Methods
XRPD. For XRPD analysis, PANalytical X-ray powder diffractometers in reflection mode were used. The XRPD parameters are listed in the table below.
Transmission
Parameters
Reflection Mode
Mode
Model
Empyrean
X’ Pert3
X’ Pert3
X-Ray wavelength
Cu, kα,
Kα1 (Å): 1.540598
Kα2 (Å): 1.544426
Kα2/Kα1 intensity ratio: 0.50
X-Ray tube setting
45 kV, 40 mA
Scan mode
Continuous
Scan range (º2 Theta)
3º-40º
Divergence slit
Automatic
1/8º
1/2º
Scan step time (s)
17.8
46.7
31.6
Step size (º2 Theta)
0.0167
0.0263
0.013
Test Time
5 min 30 s
5 min 4 s
~7 min
XRPD was also collected as follows. XRPD diffractograms were collected on a Bruker D8 diffractometer using Cu Kα radiation (40 kV, 40 mA) and a 6-28 goniometer fitted with a Ge monochromator. The incident beam passes through a 2.0 mm divergence slit followed by a 0.2 mm anti-scatter slit and knife edge. The diffracted beam passes through an 8.0 mm receiving slit with 2.5° Soller slits followed by the Lynxeye Detector. The software used for data collection and analysis was Diffrac Plus XRD Commander and Diffrac Plus EVA respectively.
Samples were run under ambient conditions as flat plate specimens using powder as received. The sample was prepared on a polished, zero-background (510) silicon wafer by gently pressing onto the flat surface or packed into a cut cavity. The sample was rotated in its own plane.
Single Crystal X-Ray Diffraction (SCXRD). Data were collected on a Rigaku Synergy Custom MM007-HF using a HyPix-6000 HPAD detector (The Woodlands, Tex., USA). Data were collected in a nitrogen gas stream at 90 K using omega scans. Data were integrated and scaled using CrysAlisPro (Rigaku Oxford Diffraction, 2021). WinGX was used for the solution and refinement of the crystal structures. Solution by iterative methods (SHELXT-2014) produced a complete heavy-atom phasing model. All non-hydrogen atoms were refined anisotropically by full-matrix least-squares (SHELXL-2018). All hydrogen atoms were placed using a riding model. Their positions were constrained relative to their parent atom using the appropriate HFIX command in SHELXL-2018.
TGA/DSC. TGA data were collected using a TA Q5000 TGA or TA Discovery TGA5500 from TA Instruments and DSC was performed using a TA Discovery DSC2500 from TA Instruments.
General Parameters for TGA and DSC Testing
Parameters
TGA
DSC
Method
Ramp
Ramp
Sample pan
Aluminum, open
Aluminum, crimped
Temperature
RT - desired temperature
25° C. - desired temperature
Heating rate
10° C./min
10° C./min
Purge gas
N2
N2
Solution NMR. Solution NMR was collected on Bruker 400M NMR Spectrometer using DMSO-d6.
Example 4—Compound A—Amorphous
Compound A (20 mg) was weighed into HPLC vials and solvent was added in 10 vol aliquots (200 μl) at RT on a stirrer plate until sample dissolution or until a maximum of 50 vol had been added and observations were made between additions. The solutions that were obtained were frozen in a dry ice acetone bath before being placed on the freeze dryer under vacuum.
Amorphous material of Compound A (mono adipate salt) was successfully prepared through freeze drying. Characterisation of the initial batch of samples were all shown to be amorphous by XRPD and the NMR's contained ca. 1.1 eq. adipic acid with varying quantities of residual solvent, except for acetonitrile/water (1:1) which contained no residual solvent. The purities were low, between 85-89%, except for 1,4-dioxane which had a very low purity of 57.5%. Static storage at 25° C./97% RH and 40° C./75% RH after 7 days were all shown to have deliquesced.
Liquid asset grinding (LAG) screens: Amorphous material (25 mg) in HPLC vials was treated with two ball bearings and solvent (5 μl, 0.2 vol) and milled on a Fritsch planetary mill fitted with an Automaxion adapter for 2 hours at 500 rpm. Samples that went into solution upon solvent addition were allowed to slowly evaporate with a needle inserted into the cap. The resultant solids from LAG were initially analysed by XRPD.
Example 4—Compound A Form A
Compound A Form A could be obtained in different solvent systems of acetone, THF, and EtOAc from screening. Single crystal data of Compound A Form A shows that Compound A Form A is anhydrous.
Compound A Form A was obtained from THF system and the sample was air dried at RT. No form change was observed before and after drying. A weight loss of 2.0% up to 100° C. was observed in TGA and DSC result showed two endotherms at 68.8° C. and 169.1° C. (peak temperature). Based on the integrals, the stoichiometric ratio of adipic acid:freebase was determined to be 1.06. Peak of THF was observed. Around 0.17 molar THF (1.9 wt %) was detected, which was consistent with TGA weight loss. The purity of Compound A Form A was 98.30 area %. After heating adipate Type A to 100° C. under N2 protection, cooled down and exposed to ambient conditions, very slight differences were observed before and after heating. Peak of THF was observed in the heated sample. Around 0.15 molar THF (1.7 wt %) was still detected, suggesting the organic solvent might be occluded in the crystal form.
VH-XRPD Analysis of Compound A. The VH-XRPD analysis performed on Compound A shows small changes between 44-46% RH which remain up until 80% RH. FIG. 19. The sample then reverts to the original form upon reaching 30% RH. The sample appears to be a channel-like hydrate system which can exist with a range of occupancies of water from 0 to around 1 eq.
Single Crystal XRD. X-ray quality crystals were grown from a saturated isopropanol solution followed by the slow vapor diffusion of heptane to deposit the crystal diffracted. A colorless prism 0.100×0.100×0.100 mm in size was mounted on a Cryoloop with Paratone oil. Data were collected in a nitrogen gas stream at 90(2) K using phi and omega scans. Crystal-to-detector distance was 40 mm and exposure time was 0.2 seconds per frame using a scan width of 1.0°. Data collection was 99.9% complete to 67.000° in θ. A total of 40537 reflections were collected covering the indices, −10<=h<=10, −15<=k<=15, −22<=l<=22. 12985 reflections were found to be symmetry independent, with an Rint of 0.0345. Indexing and unit cell refinement indicated a primitive, triclinic lattice. The space group was found to be P 1 (No. 1). The data were integrated and scaled using CrysAlisPro 1.171.40.51a. Solution by iterative methods (SHELXT-2014) produced a complete heavy-atom phasing model. All non-hydrogen atoms were refined anisotropically by full-matrix least-squares (SHELXL-2018). All hydrogen atoms were placed using a riding model. Their positions were constrained relative to their parent atom using the appropriate HFIX command in SHELXL-2018. Absolute stereochemistry was unambiguously determined from the diffraction data.
TABLE 14
Crystal data and structure refinement for Compound A Form A
Empirical formula
C35 H42 Cl F4 N7 O6
Formula weight
768.20
Temperature
90(2) K
Wavelength
1.54184 Å
Crystal system
Triclinic
Space group
P 1
Unit cell dimensions
a = 8.6289(3) Å a = 90.728(2)º.
b = 12.4836(4) Å β = 103.055(2)º.
c = 18.3690(5) Å γ = 110.167(3)º.
Volume
1800.49(10) Å3
Z
2
Density (calculated)
1.417 Mg/m3
Absorption coefficient
1.604 mm−1
F(000)
804
Crystal size
0.100 × 0.100 × 0.100 mm3
Theta range for data collection
2.481 to 75.148º
Index ranges
−10 <= h <= 10, −15 <= k <= 15,
−22 <= k <= 22
Reflections collected
40537
Independent reflections
12985 [R(int) = 0.0345]
Completeness to theta = 67.000º
99.9%
Absorption correction
Semi-empirical from equivalents
Max. and min. transmission
1.00000 and 0.84789
Refinement method
Full-matrix least-squares on F2
Data/restraints/parameters
12985/3/974
Goodness-of-fit on F2
1.089
Final R indices [I > 2sigma(I)]
R1 = 0.0471, wR2 = 0.1296
R indices (all data)
R1 = 0.0487, wR2 = 0.1310
Absolute structure parameter
0.008(14)
Extinction coefficient
0.0016(4)
Largest diff. peak and hole
0.364 and −0.309 e.Å−3
TABLE 15
Atomic coordinates (×104) and equivalent
isotropic displacement parameters (Å2 × 103)
for Compound A Form A. U(eq) is defined as one
third of the trace of the orthogonalized Uij tensor.
x
y
z
U(eq)
C(1)
561(5)
−64(3)
3149(2)
26(1)
C(2)
1896(5)
1047(3)
3157(2)
26(1)
C(3)
2296(5)
2035(3)
3650(2)
28(1)
C(4)
3565(5)
3031(3)
3580(2)
29(1)
C(5)
4519(5)
3096(3)
3048(2)
26(1)
C(6)
4192(5)
2109(3)
2613(2)
26(1)
C(7)
2903(5)
1058(3)
2650(2)
25(1)
C(8)
1564(5)
−816(3)
2294(2)
26(1)
C(9)
−1348(6)
632(3)
3713(2)
33(1)
C(10)
−3268(6)
209(4)
3364(3)
36(1)
C(11)
−3402(6)
−1761(4)
3361(2)
38(1)
C(12)
−1516(6)
−1395(3)
3739(2)
33(1)
C(13)
−1197(6)
−1450(4)
4583(3)
40(1)
C(14)
−5275(6)
−1084(4)
3994(2)
37(1)
C(15)
−5889(6)
−2210(4)
4304(3)
43(1)
C(16)
−7177(8)
−2464(5)
4619(3)
54(1)
C(17)
5723(5)
4189(3)
2868(2)
28(1)
C(18)
7476(5)
4559(3)
3083(2)
29(1)
C(19)
8434(5)
5557(3)
2790(2)
30(1)
C(20)
7546(6)
6130(3)
2338(2)
30(1)
C(21)
5756(5)
5709(3)
2144(2)
29(1)
C(22)
8421(6)
3966(3)
3618(2)
33(1)
C(23)
10347(6)
5972(4)
2929(3)
40(1)
C(24)
2289(6)
−1692(3)
1334(2)
32(1)
C(25)
1414(5)
−2762(3)
784(2)
31(1)
C(26)
2374(6)
−2759(4)
182(2)
38(1)
C(27)
1654(12)
−2118(8)
−390(5)
33(3)
C(27A)
923(13)
−3304(10)
−570(5)
47(3)
C(28)
−294(7)
−2696(5)
−440(3)
43(1)
C(29)
−1708(6)
−3895(4)
442(3)
41(1)
C(30)
−2114(6)
−1128(3)
927(2)
32(1)
C(31)
−2463(6)
−124(4)
1232(3)
36(1)
C(32)
−1359(6)
1073(4)
1105(2)
34(1)
C(33)
−1876(6)
1973(4)
1450(3)
37(1)
C(34)
−1243(6)
3160(4)
1183(3)
40(1)
C(35)
627(6)
3838(3)
1411(2)
33(1)
C(36)
7653(5)
10613(3)
6751(2)
28(1)
C(37)
7881(5)
9510(3)
6775(2)
28(1)
C(38)
6880(6)
8511(4)
6285(2)
31(1)
C(39)
7240(6)
7533(3)
6375(2)
31(1)
C(40)
8586(5)
7468(3)
6943(2)
30(1)
C(41)
9591(5)
8461(3)
7394(2)
30(1)
C(42)
9308(5)
9499(3)
7325(2)
28(1)
C(43)
10207(5)
11397(3)
7608(2)
29(1)
C(44)
4522(6)
9900(4)
6212(3)
35(1)
C(45)
3459(7)
10323(4)
6626(3)
41(1)
C(46)
5218(7)
12289(4)
6592(3)
41(1)
C(47)
6296(6)
11924(4)
6157(3)
37(1)
C(48)
5729(7)
11975(4)
5316(3)
44(1)
C(49)
2036(7)
11560(4)
5994(3)
40(1)
C(50)
2168(7)
12681(5)
5690(3)
47(1)
C(51)
787(9)
12880(6)
5368(3)
55(1)
C(52)
8898(6)
6387(3)
7130(2)
32(1)
C(53)
10055(6)
6015(3)
6897(2)
34(1)
C(54)
10344(7)
5033(4)
7197(2)
38(1)
C(55)
9368(6)
4466(3)
7672(2)
38(1)
C(56)
8175(6)
4875(4)
7867(2)
35(1)
C(57)
11028(7)
6603(4)
6348(3)
40(1)
C(58)
11690(8)
4619(4)
7040(3)
53(1)
C(59)
12759(6)
12364(3)
8545(2)
33(1)
C(60)
12137(6)
12133(4)
9265(2)
38(1)
C(61)
11813(7)
13135(5)
9591(3)
50(1)
C(62)
13569(7)
13900(4)
10070(3)
49(1)
C(63)
14632(7)
13137(5)
10203(3)
51(1)
C(64)
12720(8)
11266(5)
10444(3)
51(1)
C(65)
16230(7)
11281(5)
9132(3)
48(1)
C(66)
17137(8)
10602(6)
8843(4)
61(2)
C(67)
16592(8)
9320(6)
8949(3)
60(2)
C(68)
14934(7)
8601(5)
8435(3)
53(1)
C(69)
14320(9)
7353(6)
8609(4)
63(2)
C(70)
15286(7)
6618(5)
8437(3)
51(1)
N(1)
2756(4)
125(3)
2203(2)
26(1)
N(2)
470(4)
−973(3)
2731(2)
26(1)
N(3)
−621(5)
−228(3)
3558(2)
32(1)
N(4)
−4105(5)
−927(3)
3582(2)
36(1)
N(5)
4861(4)
4735(3)
2399(2)
28(1)
N(6)
4866(5)
6245(3)
1694(2)
34(1)
N(7)
−347(5)
−2823(3)
360(2)
33(1)
N(8)
10482(5)
10454(3)
7766(2)
31(1)
N(9)
8879(5)
11544(3)
7140(2)
30(1)
N(10)
6246(5)
10756(3)
6320(2)
33(1)
N(11)
3487(5)
11455(3)
6421(2)
39(1)
N(12)
13474(5)
11960(3)
9876(2)
39(1)
N(13)
7970(5)
5833(3)
7604(2)
33(1)
N(14)
7211(6)
4359(3)
8331(2)
44(1)
O(1)
−5807(5)
−325(3)
4122(2)
46(1)
O(2)
1324(4)
−1797(2)
1889(2)
30(1)
O(3)
−3160(5)
−2117(3)
930(2)
44(1)
O(4)
−798(4)
−932(3)
691(2)
39(1)
O(5)
1267(4)
4690(3)
1112(2)
44(1)
O(6)
1515(4)
3481(3)
1963(2)
45(1)
O(7)
668(5)
10771(3)
5860(2)
48(1)
O(8)
11360(4)
12411(2)
7968(2)
34(1)
O(9)
16640(6)
12316(4)
9040(3)
68(1)
O(10)
15093(5)
10760(3)
9474(2)
47(1)
O(11)
15259(5)
5750(3)
8737(2)
52(1)
O(12)
16106(6)
6985(4)
7918(2)
60(1)
F(1)
5128(3)
2137(2)
2117(1)
34(1)
F(2)
7403(3)
3077(2)
3890(2)
46(1)
F(3)
9380(4)
3549(2)
3302(2)
48(1)
F(4)
9486(4)
4674(2)
4213(2)
45(1)
F(5)
10905(3)
8438(2)
7938(1)
39(1)
F(6)
10771(5)
5868(3)
5752(2)
64(1)
F(7)
12714(4)
7034(3)
6630(2)
58(1)
F(8)
10602(4)
7471(3)
6067(2)
53(1)
Cl(1)
4020(1)
4261(1)
4170(1)
37(1)
Cl(2)
5988(2)
6287(1)
5777(1)
42(1)
TABLE 16
Bond lengths [Å] and angles [°] for Compound A Form A
C(1)—N(2)
1.332(5)
C(14)—C(15)
1.492(7)
C(1)—N(3)
1.361(5)
C(15)—C(16)
1.312(7)
C(1)—C(2)
1.463(5)
C(15)—H(15)
0.9500
C(2)—C(7)
1.408(5)
C(16)—H(16A)
0.9500
C(2)—C(3)
1.413(5)
C(16)—H(16B)
0.9500
C(3)—C(4)
1.374(5)
C(17)—N(5)
1.354(5)
C(3)—H(3)
0.9500
C(17)—C(18)
1.378(6)
C(4)—C(5)
1.400(6)
C(18)—C(19)
1.425(5)
C(4)—CI(1)
1.742(4)
C(18)—C(22)
1.500(5)
C(5)—C(6)
1.367(5)
C(19)—C(20)
1.377(6)
C(5)—C(17)
1.497(5)
C(19)—C(23)
1.508(6)
C(6)—F(1)
1.341(4)
C(20)—C(21)
1.405(6)
C(6)—C(7)
1.412(5)
C(20)—H(20)
0.9500
C(7)—N(1)
1.368(5)
C(21)—N(6)
1.343(5)
C(8)—N(1)
1.309(5)
C(21)—N(5)
1.351(5)
C(8)—N(2)
1.340(5)
C(22)—F(4)
1.335(5)
C(8)—O(2)
1.352(4)
C(22)—F(2)
1.340(5)
C(9)—N(3)
1.470(5)
C(22)—F(3)
1.342(5)
C(9)—C(10)
1.531(7)
C(23)—H(23A)
0.9800
C(9)—H(9A)
0.9900
C(23)—H(23B)
0.9800
C(9)—H(9B)
0.9900
C(23)—H(23C)
0.9800
C(10)—N(4)
1.460(5)
C(24)—O(2)
1.436(5)
C(10)—H(10A)
0.9900
C(24)—C(25)
1.517(5)
C(10)—H(10B)
0.9900
C(24)—H(24A)
0.9900
C(11)—N(4)
1.468(6)
C(24)—H(24B)
0.9900
C(11)—C(12)
1.520(7)
C(25)—N(7)
1.518(6)
C(11)—H(11A)
0.9900
C(25)—C(26)
1.524(6)
C(11)—H(11B)
0.9900
C(25)—H(25)
1.0000
C(12)—N(3)
1.477(5)
C(26)—C(27)
1.483(9)
C(12)—C(13)
1.518(6)
C(26)—C(27A)
1.595(10)
C(12)—H(12)
1.0000
C(26)—H(26A)
0.9900
C(13)—H(13A)
0.9800
C(26)—H(26B)
0.9900
C(13)—H(13B)
0.9800
C(27)—C(28)
1.564(11)
C(13)—H(13C)
0.9800
C(27)—H(27A)
0.9900
C(14)—O(1)
1.227(6)
C(27)—H(27B)
0.9900
C(14)—N(4)
1.357(6)
C(27A)—C(28)
1.547(11)
C(27A)—H(27C)
0.9900
C(40)—C(52)
1.494(5)
C(27A)—H(27D)
0.9900
C(41)—F(5)
1.340(5)
C(28)—N(7)
1.489(5)
C(41)—C(42)
1.401 (5)
C(28)—H(28A)
0.9900
C(42)—N(8)
1.369(5)
C(28)—H(28B)
0.9900
C(43)—N(8)
1.302(5)
C(29)—N(7)
1.482(6)
C(43)—N(9)
1.337(5)
C(29)—H(29A)
0.9800
C(43)—O(8)
1.358(5)
C(29)—H(29B)
0.9800
C(44)—N(10)
1.469(6)
C(29)—H(29C)
0.9800
C(44)—C(45)
1.528(6)
C(30)—O(4)
1.253(5)
C(44)—H(44A)
0.9900
C(30)—O(3)
1.254(5)
C(44)—H(44B)
0.9900
C(30)—C(31)
1.516(6)
C(45)—N(11)
1.461(6)
C(31)—C(32)
1.524(6)
C(45)—H(45A)
0.9900
C(31)—H(31A)
0.9900
C(45)—H(45B)
0.9900
C(31)—H(31B)
0.9900
C(46)—N(11)
1.457(7)
C(32)—C(33)
1.523(6)
C(46)—C(47)
1.526(7)
C(32)—H(32A)
0.9900
C(46)—H(46A)
0.9900
C(32)—H(32B)
0.9900
C(46)—H(46B)
0.9900
C(33)—C(34)
1.522(6)
C(47)—N(10)
1.481(5)
C(33)—H(33A)
0.9900
C(47)—C(48)
1.520(6)
C(33)—H(33B)
0.9900
C(47)—H(47)
1.0000
C(34)—C(35)
1.496(6)
C(48)—H(48A)
0.9800
C(34)—H(34A)
0.9900
C(48)—H(48B)
0.9800
C(34)—H(34B)
0.9900
C(48)—H(48C)
0.9800
C(35)—O(5)
1.217(5)
C(49)—O(7)
1.218(6)
C(35)—O(6)
1.308(5)
C(49)—N(11)
1.368(6)
C(36)—N(9)
1.331(5)
C(49)—C(50)
1.491 (7)
C(36)—N(10)
1.360(5)
C(50)—C(51)
1.312(8)
C(36)—C(37)
1.455(5)
C(50)—H(50)
0.9500
C(37)—C(42)
1.410(6)
C(51)—H(51A)
0.9500
C(37)—C(38)
1.410(6)
C(51)—H(51B)
0.9500
C(38)—C(39)
1.362(6)
C(52)—N(13)
1.350(5)
C(38)—H(38)
0.9500
C(52)—C(53)
1.380(6)
C(39)—C(40)
1.402(6)
C(53)—C(54)
1.427(6)
C(39)—CI(2)
1.748(4)
C(53)—C(57)
1.495(6)
C(40)—C(41)
1.372(6)
C(54)—C(55)
1.381(6)
C(54)—C(58)
1.504(7)
C(66)—H(66B)
0.9900
C(55)—C(56)
1.405(7)
C(67)—C(68)
1.492(9)
C(55)—H(55)
0.9500
C(67)—H(67A)
0.9900
C(56)—N(14)
1.339(6)
C(67)—H(67B)
0.9900
C(56)—N(13)
1.349(6)
C(68)—C(69)
1.527(9)
C(57)—F(8)
1.333(5)
C(68)—H(68A)
0.9900
C(57)—F(7)
1.337(6)
C(68)—H(68B)
0.9900
C(57)—F(6)
1.347(5)
C(69)—C(70)
1.507(8)
C(58)—H(58A)
0.9800
C(69)—H(69A)
0.9900
C(58)—H(58B)
0.9800
C(69)—H(69B)
0.9900
C(58)—H(58C)
0.9800
C(70)—O(11)
1.218(7)
C(59)—O(8)
1.434(5)
C(70)—O(12)
1.308(6)
C(59)—C(60)
1.530(6)
N(6)—H(6A)
0.8800
C(59)—H(59A)
0.9900
N(6)—H(6B)
0.8800
C(59)—H(59B)
0.9900
N(7)—H(7)
1.0000
C(60)—N(12)
1.493(6)
N(12)—H(12)
1.0000
C(60)—C(61)
1.516(6)
N(14)—H(14A)
0.8800
C(60)—H(60)
1.0000
N(14)—H(14B)
0.8800
C(61)—C(62)
1.537(8)
O(6)—H(6)
0.8400
C(61)—H(61A)
0.9900
O(12)—H(12A)
0.8400
C(61)—H(61B)
0.9900
N(2)—C(1)—N(3)
117.0(3)
C(62)—C(63)
1.521(7)
N(2)—C(1)—C(2)
120.0(3)
C(62)—H(62A)
0.9900
N(3)—C(1)—C(2)
123.0(3)
C(62)—H(62B)
0.9900
C(7)—C(2)—C(3)
119.8(3)
C(63)—N(12)
1.488(6)
C(7)—C(2)—C(1)
114.1(3)
C(63)—H(63A)
0.9900
C(3)—C(2)—C(1)
126.0(3)
C(63)—H(63B)
0.9900
C(4)—C(3)—C(2)
119.5(4)
C(64)—N(12)
1.484(6)
C(4)—C(3)—H(3)
120.2
C(64)—H(64A)
0.9800
C(2)—C(3)—H(3)
120.2
C(64)—H(64B)
0.9800
C(3)—C(4)—C(5)
122.2(3)
C(64)—H(64C)
0.9800
C(3)—C(4)—CI(1)
119.6(3)
C(65)—O(9)
1.242(7)
C(5)—C(4)—CI(1)
118.3(3)
C(65)—O(10)
1.276(6)
C(6)—C(5)—C(4)
117.3(3)
C(65)—C(66)
1.499(8)
C(6)—C(5)—C(17)
118.0(3)
C(66)—C(67)
1.534(10)
C(4)—C(5)—C(17)
124.3(3)
C(66)—H(66A)
0.9900
F(1)—C(6)—C(5)
118.6(3)
F(1)—C(6)—C(7)
117.8(3)
H(13A)—C(13)—H(13C)
109.5
C(5)—C(6)—C(7)
123.6(3)
H(13B)—C(13)—H(13C)
109.5
N(1)—C(7)—C(2)
125.2(3)
O(1)—C(14)—N(4)
121.8(4)
N(1)—C(7)—C(6)
117.5(3)
O(1)—C(14)—C(15)
120.1(4)
C(2)—C(7)—C(6)
117.3(3)
N(4)—C(14)—C(15)
118.0(4)
N(1)—C(8)—N(2)
129.6(3)
C(16)—C(15)—C(14)
120.5(5)
N(1)—C(8)—O(2)
118.2(3)
C(16)—C(15)—H(15)
119.8
N(2)—C(8)—O(2)
112.1(3)
C(14)—C(15)—H(15)
119.8
N(3)—C(9)—C(10)
111.3(3)
C(15)—C(16)—H(16A)
120.0
N(3)—C(9)—H(9A)
109.4
C(15)—C(16)—H(16B)
120.0
C(10)—C(9)—H(9A)
109.4
H(16A)—C(16)—H(16B)
120.0
N(3)—C(9)—H(9B)
109.4
N(5)—C(17)—C(18)
123.3(3)
C(10)—C(9)—H(9B)
109.4
N(5)—C(17)—C(5)
110.6(3)
H(9A)—C(9)—H(9B)
108.0
C(18)—C(17)—C(5)
125.9(3)
N(4)—C(10)—C(9)
110.5(4)
C(17)—C(18)—C(19)
118.6(4)
N(4)—C(10)—H(10A)
109.5
C(17)—C(18)—C(22)
122.9(3)
C(9)—C(10)—H(10A)
109.5
C(19)—C(18)—C(22)
118.5(4)
N(4)—C(10)—H(10B)
109.5
C(20)—C(19)—C(18)
117.6(4)
C(9)—C(10)—H(10B)
109.5
C(20)—C(19)—C(23)
119.4(4)
H(10A)—C(10)—H(10B)
108.1
C(18)—C(19)—C(23)
123.0(4)
N(4)—C(11)—C(12)
110.5(3)
C(19)—C(20)—C(21)
120.8(4)
N(4)—C(11)—H(11A)
109.5
C(19)—C(20)—H(20)
119.6
C(12)—C(11)—H(11A)
109.5
C(21)—C(20)—H(20)
119.6
N(4)—C(11)—H(11B)
109.5
N(6)—C(21)—N(5)
117.3(4)
C(12)—C(11)—H(11B)
109.5
N(6)—C(21)—C(20)
121.7(3)
H(11A)—C(11)—H(11B)
108.1
N(5)—C(21)—C(20)
121.0(3)
N(3)—C(12)—C(13)
111.0(4)
F(4)—C(22)—F(2)
106.2(3)
N(3)—C(12)—C(11)
109.3(3)
F(4)—C(22)—F(3)
105.9(4)
C(13)—C(12)—C(11)
112.1(4)
F(2)—C(22)—F(3)
105.9(3)
N(3)—C(12)—H(12)
108.1
F(4)—C(22)—C(18)
112.0(3)
C(13)—C(12)—H(12)
108.1
F(2)—C(22)—C(18)
113.7(4)
C(11)—C(12)—H(12)
108.1
F(3)—C(22)—C(18)
112.5(3)
C(12)—C(13)—H(13A)
109.5
C(19)—C(23)—H(23A)
109.5
C(12)—C(13)—H(13B)
109.5
C(19)—C(23)—H(23B)
109.5
H(13A)—C(13)—H(13B)
109.5
H(23A)—C(23)—H(23B)
109.5
C(12)—C(13)—H(13C)
109.5
C(19)—C(23)—H(23C)
109.5
H(23A)—C(23)—H(23C)
109.5
C(27)—C(28)—H(28A)
111.2
H(23B)—C(23)—H(23C)
109.5
N(7)—C(28)—H(28B)
111.2
O(2)—C(24)—C(25)
107.2(3)
C(27)—C(28)—H(28B)
111.2
O(2)—C(24)—H(24A)
110.3
H(28A)—C(28)—H(28B)
109.1
C(25)—C(24)—H(24A)
110.3
N(7)—C(29)—H(29A)
109.5
O(2)—C(24)—H(24B)
110.3
N(7)—C(29)—H(29B)
109.5
C(25)—C(24)—H(24B)
110.3
H(29A)—C(29)—H(29B)
109.5
H(24A)—C(24)—H(24B)
108.5
N(7)—C(29)—H(29C)
109.5
C(24)—C(25)—N(7)
110.9(3)
H(29A)—C(29)—H(29C)
109.5
C(24)—C(25)—C(26)
111.6(4)
H(29B)—C(29)—H(29C)
109.5
N(7)—C(25)—C(26)
105.2(3)
O(4)—C(30)—O(3)
123.6(4)
C(24)—C(25)—H(25)
109.7
O(4)—C(30)—C(31)
118.7(4)
N(7)—C(25)—H(25)
109.7
O(3)—C(30)—C(31)
117.8(4)
C(26)—C(25)—H(25)
109.7
C(30)—C(31)—C(32)
117.2(4)
C(27)—C(26)—C(25)
102.2(4)
C(30)—C(31)—H(31A)
108.0
C(25)—C(26)—C(27A)
104.8(5)
C(32)—C(31)—H(31A)
108.0
C(27)—C(26)—H(26A)
111.3
C(30)—C(31)—H(31B)
108.0
C(25)—C(26)—H(26A)
111.3
C(32)—C(31)—H(31B)
108.0
C(27)—C(26)—H(26B)
111.3
H(31A)—C(31)—H(31B)
107.2
C(25)—C(26)—H(26B)
111.3
C(33)—C(32)—C(31)
110.1(4)
H(26A)—C(26)—H(26B)
109.2
C(33)—C(32)—H(32A)
109.6
C(26)—C(27)—C(28)
101.2(6)
C(31)—C(32)—H(32A)
109.6
C(26)—C(27)—H(27A)
111.5
C(33)—C(32)—H(32B)
109.6
C(28)—C(27)—H(27A)
111.5
C(31)—C(32)—H(32B)
109.6
C(26)—C(27)—H(27B)
111.5
H(32A)—C(32)—H(32B)
108.1
C(28)—C(27)—H(27B)
111.5
C(34)—C(33)—C(32)
115.4(4)
H(27A)—C(27)—H(27B)
109.3
C(34)—C(33)—H(33A)
108.4
C(28)—C(27A)—C(26)
97.1(5)
C(32)—C(33)—H(33A)
108.4
C(28)—C(27A)—H(27C)
112.3
C(34)—C(33)—H(33B)
108.4
C(26)—C(27A)—H(27C)
112.3
C(32)—C(33)—H(33B)
108.4
C(28)—C(27A)—H(27D)
112.3
H(33A)—C(33)—H(33B)
107.5
C(26)—C(27A)—H(27D)
112.3
C(35)—C(34)—C(33)
118.1(4)
H(27C)—C(27A)—H(27D)
109.9
C(35)—C(34)—H(34A)
107.8
N(7)—C(28)—C(27A)
104.3(5)
C(33)—C(34)—H(34A)
107.8
N(7)—C(28)—C(27)
103.0(4)
C(35)—C(34)—H(34B)
107.8
N(7)—C(28)—H(28A)
111.2
C(33)—C(34)—H(34B)
107.8
H(34A)—C(34)—H(34B)
107.1
C(44)—C(45)—H(45A)
109.5
O(5)—C(35)—O(6)
122.3(4)
N(11)—C(45)—H(45B)
109.5
O(5)—C(35)—C(34)
121.7(4)
C(44)—C(45)—H(45B)
109.5
O(6)—C(35)—C(34)
116.0(4)
H(45A)—C(45)—H(45B)
108.1
N(9)—C(36)—N(10)
117.1(3)
N(11)—C(46)—C(47)
110.5(4)
N(9)—C(36)—C(37)
120.0(4)
N(11)—C(46)—H(46A)
109.5
N(10)—C(36)—C(37)
122.8(4)
C(47)—C(46)—H(46A)
109.5
C(42)—C(37)—C(38)
119.1(3)
N(11)—C(46)—H(46B)
109.5
C(42)—C(37)—C(36)
114.5(4)
C(47)—C(46)—H(46B)
109.5
C(38)—C(37)—C(36)
126.3(4)
H(46A)—C(46)—H(46B)
108.1
C(39)—C(38)—C(37)
120.0(4)
N(10)—C(47)—C(48)
110.5(4)
C(39)—C(38)—H(38)
120.0
N(10)—C(47)—C(46)
109.7(4)
C(37)—C(38)—H(38)
120.0
C(48)—C(47)—C(46)
112.3(4)
C(38)—C(39)—C(40)
122.6(4)
N(10)—C(47)—H(47)
108.0
C(38)—C(39)—CI(2)
120.2(3)
C(48)—C(47)—H(47)
108.0
C(40)—C(39)—CI(2)
117.2(3)
C(46)—C(47)—H(47)
108.0
C(41)—C(40)—C(39)
116.6(4)
C(47)—C(48)—H(48A)
109.5
C(41)—C(40)—C(52)
118.4(4)
C(47)—C(48)—H(48B)
109.5
C(39)—C(40)—C(52)
124.8(4)
H(48A)—C(48)—H(48B)
109.5
F(5)—C(41)—C(40)
118.5(3)
C(47)—C(48)—H(48C)
109.5
F(5)—C(41)—C(42)
117.9(3)
H(48A)—C(48)—H(48C)
109.5
C(40)—C(41)—C(42)
123.6(4)
H(48B)—C(48)—H(48C)
109.5
N(8)—C(42)—C(41)
118.2(4)
O(7)—C(49)—N(11)
122.0(5)
N(8)—C(42)—C(37)
123.8(3)
O(7)—C(49)—C(50)
120.2(5)
C(41)—C(42)—C(37)
117.9(4)
N(11)—C(49)—C(50)
117.9(5)
N(8)—C(43)—N(9)
129.6(4)
C(51)—C(50)—C(49)
120.2(6)
N(8)—C(43)—O(8)
119.0(4)
C(51)—C(50)—H(50)
119.9
N(9)—C(43)—O(8)
111.4(3)
C(49)—C(50)—H(50)
119.9
N(10)—C(44)—C(45)
111.2(4)
C(50)—C(51)—H(51A)
120.0
N(10)—C(44)—H(44A)
109.4
C(50)—C(51)—H(51B)
120.0
C(45)—C(44)—H(44A)
109.4
H(51A)—C(51)—H(51B)
120.0
N(10)—C(44)—H(44B)
109.4
N(13)—C(52)—C(53)
123.0(4)
C(45)—C(44)—H(44B)
109.4
N(13)—C(52)—C(40)
111.4(3)
H(44A)—C(44)—H(44B)
108.0
C(53)—C(52)—C(40)
125.5(4)
N(11)—C(45)—C(44)
110.6(4)
C(52)—C(53)—C(54)
118.5(4)
N(11)—C(45)—H(45A)
109.5
C(52)—C(53)—C(57)
122.8(4)
C(54)—C(53)—C(57)
118.7(4)
C(62)—C(61)—H(61A)
110.9
C(55)—C(54)—C(53)
117.8(4)
C(60)—C(61)—H(61B)
110.9
C(55)—C(54)—C(58)
119.1(4)
C(62)—C(61)—H(61B)
110.9
C(53)—C(54)—C(58)
123.1(4)
H(61A)—C(61)—H(61B)
109.0
C(54)—C(55)—C(56)
120.5(4)
C(63)—C(62)—C(61)
105.7(4)
C(54)—C(55)—H(55)
119.7
C(63)—C(62)—H(62A)
110.6
C(56)—C(55)—H(55)
119.7
C(61)—C(62)—H(62A)
110.6
N(14)—C(56)—N(13)
116.5(4)
C(63)—C(62)—H(62B)
110.6
N(14)—C(56)—C(55)
122.6(4)
C(61)—C(62)—H(62B)
110.6
N(13)—C(56)—C(55)
120.9(4)
H(62A)—C(62)—H(62B)
108.7
F(8)—C(57)—F(7)
105.8(4)
N(12)—C(63)—C(62)
106.7(4)
F(8)—C(57)—F(6)
105.8(4)
N(12)—C(63)—H(63A)
110.4
F(7)—C(57)—F(6)
105.5(4)
C(62)—C(63)—H(63A)
110.4
F(8)—C(57)—C(53)
114.3(4)
N(12)—C(63)—H(63B)
110.4
F(7)—C(57)—C(53)
113.8(4)
C(62)—C(63)—H(63B)
110.4
F(6)—C(57)—C(53)
110.9(4)
H(63A)—C(63)—H(63B)
108.6
C(54)—C(58)—H(58A)
109.5
N(12)—C(64)—H(64A)
109.5
C(54)—C(58)—H(58B)
109.5
N(12)—C(64)—H(64B)
109.5
H(58A)—C(58)—H(58B)
109.5
H(64A)—C(64)—H(64B)
109.5
C(54)—C(58)—H(58C)
109.5
N(12)—C(64)—H(64C)
109.5
H(58A)—C(58)—H(58C)
109.5
H(64A)—C(64)—H(64C)
109.5
H(58B)—C(58)—H(58C)
109.5
H(64B)—C(64)—H(64C)
109.5
O(8)—C(59)—C(60)
107.4(4)
O(9)—C(65)—O(10)
123.6(5)
O(8)—C(59)—H(59A)
110.2
O(9)—C(65)—C(66)
118.6(5)
C(60)—C(59)—H(59A)
110.2
O(10)—C(65)—C(66)
117.7(5)
O(8)—C(59)—H(59B)
110.2
C(65)—C(66)—C(67)
118.0(5)
C(60)—C(59)—H(59B)
110.2
C(65)—C(66)—H(66A)
107.8
H(59A)—C(59)—H(59B)
108.5
C(67)—C(66)—H(66A)
107.8
N(12)—C(60)—C(61)
103.8(4)
C(65)—C(66)—H(66B)
107.8
N(12)—C(60)—C(59)
110.5(4)
C(67)—C(66)—H(66B)
107.8
C(61)—C(60)—C(59)
113.4(4)
H(66A)—C(66)—H(66B)
107.1
N(12)—C(60)—H(60)
109.6
C(68)—C(67)—C(66)
114.2(5)
C(61)—C(60)—H(60)
109.6
C(68)—C(67)—H(67A)
108.7
C(59)—C(60)—H(60)
109.6
C(66)—C(67)—H(67A)
108.7
C(60)—C(61)—C(62)
104.1(4)
C(68)—C(67)—H(67B)
108.7
C(60)—C(61)—H(61A)
110.9
C(66)—C(67)—H(67B)
108.7
H(67A)—C(67)—H(67B)
107.6
C(29)—N(7)—C(28)
111.8(4)
C(67)—C(68)—C(69)
113.2(5)
C(29)—N(7)—C(25)
112.7(3)
C(67)—C(68)—H(68A)
108.9
C(28)—N(7)—C(25)
106.8(3)
C(69)—C(68)—H(68A)
108.9
C(29)—N(7)—H(7)
108.5
C(67)—C(68)—H(68B)
108.9
C(28)—N(7)—H(7)
108.5
C(69)—C(68)—H(68B)
108.9
C(25)—N(7)—H(7)
108.5
H(68A)—C(68)—H(68B)
107.7
C(43)—N(8)—C(42)
113.7(3)
C(70)—C(69)—C(68)
117.6(5)
C(36)—N(9)—C(43)
117.4(3)
C(70)—C(69)—H(69A)
107.9
C(36)—N(10)—C(44)
122.9(3)
C(68)—C(69)—H(69A)
107.9
C(36)—N(10)—C(47)
119.6(3)
C(70)—C(69)—H(69B)
107.9
C(44)—N(10)—C(47)
114.4(3)
C(68)—C(69)—H(69B)
107.9
C(49)—N(11)—C(46)
128.3(4)
H(69A)—C(69)—H(69B)
107.2
C(49)—N(11)—C(45)
119.1(4)
O(11)—C(70)—O(12)
123.5(5)
C(46)—N(11)—C(45)
111.4(4)
O(11)—C(70)—C(69)
123.1(5)
C(64)—N(12)—C(63)
112.0(4)
O(12)—C(70)—C(69)
113.4(5)
C(64)—N(12)—C(60)
111.5(4)
C(8)—N(1)—C(7)
113.1(3)
C(63)—N(12)—C(60)
104.8(4)
C(1)—N(2)—C(8)
117.9(3)
C(64)—N(12)—H(12)
109.5
C(1)—N(3)—C(9)
124.3(3)
C(63)—N(12)—H(12)
109.5
C(1)—N(3)—C(12)
119.6(3)
C(60)—N(12)—H(12)
109.5
C(9)—N(3)—C(12)
114.9(3)
C(56)—N(13)—C(52)
119.2(4)
C(14)—N(4)—C(10)
120.2(4)
C(56)—N(14)—H(14A)
120.0
C(14)—N(4)—C(11)
128.0(4)
C(56)—N(14)—H(14B)
120.0
C(10)—N(4)—C(11)
111.6(3)
H(14A)—N(14)—H(14B)
120.0
C(21)—N(5)—C(17)
118.6(4)
C(8)—O(2)—C(24)
116.3(3)
C(21)—N(6)—H(6A)
120.0
C(35)—O(6)—H(6)
109.5
C(21)—N(6)—H(6B)
120.0
C(43)—O(8)—C(59)
117.1(3)
H(6A)—N(6)—H(6B)
120.0
C(70)—O(12)—H(12A)
109.5
TABLE 17
Anisotropic displacement parameters (Å2 × 103) for Compound A
Form A. The anisotropic displacement factor exponent takes the
form: −2π2[ h2a*2U11 + . . . + 2 h k a* b* U12]
U11
U22
U33
U23
U13
U12
C(1)
30(2)
20(2)
27(2)
3(1)
6(2)
6(2)
C(2)
28(2)
20(2)
27(2)
2(1)
4(2)
6(2)
C(3)
31(2)
22(2)
27(2)
0(1)
7(2)
6(2)
C(4)
34(2)
20(2)
29(2)
0(1)
4(2)
7(2)
C(5)
27(2)
20(2)
26(2)
2(1)
1(2)
5(2)
C(6)
28(2)
19(2)
29(2)
2(1)
7(2)
6(2)
C(7)
28(2)
18(2)
26(2)
2(1)
4(2)
5(2)
C(8)
32(2)
17(2)
26(2)
1(1)
5(2)
6(2)
C(9)
38(2)
22(2)
40(2)
1 (2)
16(2)
8(2)
C(10)
37(2)
32(2)
39(2)
5(2)
12(2)
10(2)
C(11)
48(3)
25(2)
37(2)
0(2)
17(2)
5(2)
C(12)
40(2)
24(2)
39(2)
7(2)
19(2)
8(2)
C(13)
43(3)
35(2)
42(2)
11(2)
13(2)
12(2)
C(14)
29(2)
41(2)
31(2)
−2(2)
2(2)
5(2)
C(15)
39(3)
43(2)
37(2)
0(2)
9(2)
1(2)
C(16)
55(3)
53(3)
38(2)
−4(2)
17(2)
−1(3)
C(17)
33(2)
18(2)
28(2)
0(1)
5(2)
5(2)
C(18)
31(2)
20(2)
29(2)
1(1)
2(2)
5(2)
C(19)
31(2)
20(2)
31(2)
−1(1)
4(2)
2(2)
C(20)
36(2)
17(2)
31(2)
1(1)
5(2)
4(2)
C(21)
35(2)
16(2)
29(2)
0(1)
4(2)
5(2)
C(22)
32(2)
24(2)
34(2)
5(2)
2(2)
1(2)
C(23)
35(2)
31(2)
46(2)
9(2)
5(2)
5(2)
C(24)
36(2)
23(2)
36(2)
−1(2)
11(2)
7(2)
C(25)
36(2)
24(2)
32(2)
1(2)
8(2)
11(2)
C(26)
42(3)
39(2)
36(2)
−2(2)
9(2)
17(2)
C(27)
38(5)
42(5)
26(4)
4(3)
10(3)
21(4)
C(27A)
45(6)
58(6)
32(4)
−12(4)
4(4)
15(5)
C(28)
46(3)
58(3)
33(2)
10(2)
10(2)
28(2)
C(29)
38(3)
31(2)
47(2)
−2(2)
11(2)
4(2)
C(30)
35(2)
26(2)
34(2)
4(2)
8(2)
11(2)
C(31)
37(2)
30(2)
42(2)
2(2)
12(2)
12(2)
C(32)
31(2)
29(2)
39(2)
−1(2)
7(2)
9(2)
C(33)
30(2)
31(2)
48(2)
−3(2)
9(2)
9(2)
C(34)
32(2)
30(2)
54(3)
−3(2)
3(2)
12(2)
C(35)
33(2)
24(2)
41(2)
−2(2)
2(2)
12(2)
C(36)
31(2)
26(2)
28(2)
3(1)
10(2)
10(2)
C(37)
32(2)
26(2)
27(2)
2(1)
8(2)
10(2)
C(38)
32(2)
31(2)
26(2)
2(2)
5(2)
9(2)
C(39)
37(2)
24(2)
25(2)
−3(1)
7(2)
6(2)
C(40)
35(2)
25(2)
31(2)
0(2)
10(2)
10(2)
C(41)
30(2)
27(2)
31(2)
1(2)
3(2)
11(2)
C(42)
32(2)
24(2)
27(2)
1(1)
7(2)
11(2)
C(43)
32(2)
23(2)
29(2)
1(1)
6(2)
9(2)
C(44)
31(2)
26(2)
42(2)
−1(2)
2(2)
7(2)
C(45)
44(3)
33(2)
50(3)
7(2)
14(2)
14(2)
C(46)
50(3)
29(2)
39(2)
1(2)
1 (2)
16(2)
C(47)
36(2)
28(2)
42(2)
8(2)
0(2)
11(2)
C(48)
50(3)
46(3)
42(2)
15(2)
12(2)
22(2)
C(49)
45(3)
43(2)
38(2)
−2(2)
15(2)
20(2)
C(50)
54(3)
48(3)
46(3)
3(2)
11(2)
27(2)
C(51)
72(4)
63(3)
37(2)
−4(2)
0(2)
40(3)
C(52)
39(2)
23(2)
28(2)
−2(1)
7(2)
7(2)
C(53)
44(3)
20(2)
38(2)
2(2)
14(2)
11(2)
C(54)
55(3)
24(2)
36(2)
3(2)
15(2)
14(2)
C(55)
53(3)
23(2)
36(2)
4(2)
12(2)
12(2)
C(56)
45(3)
27(2)
28(2)
1(2)
9(2)
7(2)
C(57)
59(3)
28(2)
44(2)
7(2)
26(2)
21(2)
C(58)
79(4)
35(2)
66(3)
17(2)
38(3)
31(3)
C(59)
33(2)
24(2)
35(2)
0(2)
1(2)
8(2)
C(60)
34(2)
38(2)
37(2)
−4(2)
3(2)
12(2)
C(61)
50(3)
53(3)
47(3)
−11(2)
4(2)
26(2)
C(62)
55(3)
40(2)
50(3)
−9(2)
10(2)
16(2)
C(63)
44(3)
40(3)
58(3)
−3(2)
−2(2)
10(2)
C(64)
52(3)
52(3)
51(3)
13(2)
18(2)
19(2)
C(65)
42(3)
63(3)
41(2)
15(2)
11(2)
22(2)
C(66)
46(3)
86(4)
54(3)
−2(3)
19(3)
22(3)
C(67)
57(4)
89(4)
50(3)
−4(3)
9(3)
48(3)
C(68)
53(3)
72(4)
44(3)
2(2)
13(2)
34(3)
C(69)
68(4)
76(4)
65(3)
14(3)
37(3)
36(3)
C(70)
50(3)
61(3)
48(3)
4(2)
18(2)
24(3)
N(1)
28(2)
19(1)
28(2)
1(1)
6(1)
4(1)
N(2)
30(2)
19(1)
28(2)
1(1)
7(1)
5(1)
N(3)
37(2)
18(2)
41(2)
5(1)
17(2)
8(1)
N(4)
36(2)
29(2)
37(2)
2(1)
10(2)
4(2)
N(5)
32(2)
18(1)
30(2)
2(1)
5(1)
6(1)
N(6)
34(2)
21(2)
41(2)
6(1)
2(2)
7(1)
N(7)
37(2)
28(2)
34(2)
0(1)
9(2)
12(2)
N(8)
36(2)
24(2)
30(2)
2(1)
4(1)
11(1)
N(9)
33(2)
26(2)
30(2)
2(1)
6(1)
11(1)
N(10)
31(2)
24(2)
38(2)
5(1)
2(2)
8(1)
N(11)
42(2)
32(2)
45(2)
4(2)
9(2)
16(2)
N(12)
38(2)
35(2)
39(2)
3(2)
8(2)
10(2)
N(13)
39(2)
26(2)
31(2)
0(1)
9(2)
8(2)
N(14)
57(3)
36(2)
43(2)
11(2)
22(2)
15(2)
O(1)
43(2)
54(2)
47(2)
5(2)
17(2)
19(2)
O(2)
37(2)
18(1)
32(1)
0(1)
11(1)
5(1)
O(3)
46(2)
28(2)
55(2)
8(1)
16(2)
9(1)
O(4)
39(2)
29(1)
49(2)
2(1)
13(1)
11(1)
O(5)
41(2)
29(2)
54(2)
9(1)
0(2)
10(1)
O(6)
33(2)
36(2)
54(2)
14(2)
−1(2)
5(1)
O(7)
41(2)
52(2)
50(2)
−2(2)
9(2)
17(2)
O(8)
36(2)
22(1)
37(1)
0(1)
−3(1)
8(1)
O(9)
63(3)
70(3)
84(3)
37(2)
34(2)
28(2)
O(10)
50(2)
52(2)
47(2)
10(2)
18(2)
23(2)
O(11)
56(2)
59(2)
47(2)
11(2)
23(2)
22(2)
O(12)
79(3)
74(3)
60(2)
28(2)
44(2)
50(2)
F(1)
39(1)
22(1)
39(1)
0(1)
19(1)
3(1)
F(2)
37(2)
34(1)
54(2)
24(1)
1(1)
3(1)
F(3)
48(2)
43(2)
57(2)
11(1)
9(1)
25(1)
F(4)
47(2)
33(1)
38(1)
0(1)
−12(1)
6(1)
F(5)
41(1)
25(1)
46(1)
0(1)
−4(1)
14(1)
F(6)
107(3)
39(2)
56(2)
1(1)
51(2)
17(2)
F(7)
54(2)
55(2)
71(2)
22(2)
30(2)
17(2)
F(8)
77(2)
45(2)
63(2)
31(1)
43(2)
36(2)
Cl(1)
48(1)
22(1)
36(1)
−6(1)
12(1)
5(1)
Cl(2)
55(1)
26(1)
36(1)
−8(1)
0(1)
10(1)
TABLE 18
Hydrogen coordinates (×104) and isotropic
displacement parameters (Å2 × 103) for
Compound A Form A
x
y
z
U(eq)
H(3)
1693
2012
4026
33
H(9A)
−784
1352
3506
39
H(9B)
−1128
799
4262
39
H(10A)
−3749
754
3534
43
H(10B)
−3483
176
2811
43
H(11A)
−3566
−1822
2808
45
H(11B)
−4016
−2524
3504
45
H(12)
−1056
−1930
3529
40
H(13A)
32
−1203
4804
60
H(13B)
−1753
−2239
4689
60
H(13C)
−1662
−943
4799
60
H(15)
−5344
−2747
4274
52
H(16A)
−7726
−1929
4650
64
H(16B)
−7562
−3183
4815
64
H(20)
8150
6819
2154
36
H(23A)
10662
5511
2593
60
H(23B)
10845
5897
3452
60
H(23C)
10776
6779
2831
60
H(24A)
3472
−1624
1575
38
H(24B)
2323
−1000
1070
38
H(26A)
1319
−3458
1061
37
H(26A)
3616
−2363
381
46
H(26B)
2149
−3549
−26
46
H(27A)
1917
−2223
−877
39
H(27B)
2077
−1289
−222
39
H(27C)
1338
3090
−1027
57
H(27D)
401
−4149
−590
5
H(28A)
−924
−2203
−663
52
H(28B)
−779
−3451
−741
52
H(29A)
−2815
−3890
160
61
H(29B)
−1706
−3948
974
61
H(29C)
−1505
−4555
247
61
H(31A)
−2335
−159
1780
43
H(31B)
−3667
−228
1006
43
H(32A)
−147
1205
1337
40
H(32B)
−1491
1138
560
40
H(33A)
−3135
1698
1338
44
H(33B)
−1446
2042
2003
44
H(34A)
−1598
3072
627
48
H(34B)
−1839
3620
1363
48
H(38)
5956
8520
5893
37
H(44A)
4597
9176
6401
42
H(44B)
3956
9741
5670
42
H(45A)
2269
9774
6497
50
H(45B)
3917
10362
7175
50
H(46A)
5735
12357
7138
49
H(46B)
5194
13050
6457
49
H(47)
7501
12464
6336
44
H(48A)
6429
11710
5059
66
H(48B)
5861
12766
5215
66
H(48C)
4531
11481
5133
66
H(50)
3256
13252
5729
57
H(51A)
−302
12310
5329
66
H(51B)
877
13595
5175
66
H(55)
9504
3795
7867
45
H(58A)
11988
4157
7438
80
H(58B)
12704
5279
7025
80
H(58C)
11255
4151
6555
80
H(59A)
13732
13100
8622
39
H(59B)
13134
11743
8403
39
H(60)
11077
11436
9166
45
H(61A)
10983
12871
9904
60
H(61B)
11374
13550
9188
60
H(62A)
14095
14559
9801
59
H(62B)
13468
14196
10553
59
H(63A)
15587
13411
9956
61
H(63B)
15106
13145
10748
61
H(64A)
13585
11037
10778
76
H(64B)
11764
10580
10189
76
H(64C)
12312
11723
10739
76
H(66B)
18366
10963
9088
74
H(66B)
17005
10680
8299
74
H(67A)
17488
9039
8868
72
H(67B)
16509
9219
9474
72
H(68A)
15055
8626
7912
63
H(68B)
14062
8933
8473
63
H(69A)
14340
7347
9150
76
H(69B)
13117
6984
8326
76
H(6A)
3746
5959
1576
41
H(6B)
5403
6882
1516
41
H(7)
−576
−2158
559
40
H(12)
14118
11567
9654
46
H(14A)
6493
4649
8448
53
H(14B)
7297
3731
8518
53
H(6)
2554
3875
2029
67
H(12A)
16607
6541
7840
90
Example 5—Compound A Form D
The crystal structure of Compound A Form D was determined using X-ray data collected at 100 K on a crystal isolated from the batch. The structure of Compound A Form D was solved and refined in the non-centrosymmetric, monoclinic space group l2 with the final R1[l>2σ(l)]=3.54%. The asymmetric unit was found to contain one molecule of Compound A, one fully ordered adipate anion, one 50% occupied water molecule (O7), which is positioned on a crystallographic special position (2-fold axis) and one partially occupied water molecule (O8, 20% occupancy) disordered about a special position (2-fold axis). In the structure, the molecule also shows positional disorder with the methylpyrrolidine ring disordered over two sites and modelled with a 64.6:35.4 ratio. The absolute stereochemistry of the compound has been determined with stereocentres C6 and C25 in the S configuration. The Flack parameter for this structure is 0.007(8). The XRPD pattern simulated from the crystal structure data (collected at 100 K) is consistent with the reference experimental diffractogram of Form D (collected at RT). Slight differences in the simulated and experimental diffractograms are attributable to lattice variations with temperature and preferred orientation.
An overlay with calculated diffractogram of hydrated Form D shows that calculated XRPDs of these two Forms are similar, however there are some differences. The simulated diffractogram is consistent with the experimental VH diffractogram of Compound A Form A at 10% RH. Slight differences in the simulated and experimental diffractograms are attributable to lattice variations with temperature and preferred orientation.
Compound A Form A, C and D are structurally similar and interconvert rapidly depending upon the ambient relative humidity with the majority of water uptake occurring between 40-50% RH at 25° C.
Transitions of Forms of Compound A at varying RH.
% Relative Humidity
XRPD
0%-44%
Compound A Form A
49%-54%
Transition
58%-76%-49%
Compound A Form D
44%
Transition
39%-0%-44%
Compound A Form A
49%
Transition
54%-76%-53%
Compound A Form D
48%
Transition
44%-0%
Compound A Form A
Single crystal experiments. The single crystal X-ray structure of Compound A Form D was determined at 100 K using a crystal grown by slow evaporation from THF. A crystal of sufficient size and quality for analysis by single crystal X-ray diffraction was isolated with approximate dimensions 0.22×0.20×0.08 mm.
The crystals were monoclinic, group l2 with the final R1=[l>2σ(l)]=3.54%. The compound was confirmed as Compound A Form D. The asymmetric unit contained one molecule of Compound A Form D, one fully ordered adipate anion, one 50% occupied water molecule, O7, sitting on a crystallographic special position (2-fold axis) and one partially occupied water molecule, O8, disordered about a special position (2-fold axis). The refined atomic occupancy of O8 is 0.195 (approximately 20% water). The molecule also showed positional disorder at carbon C27 methylpyrrolidine ring which has been modelled over two sites with a 64.6:35.4 ratio.
TABLE 19
Crystal data and structure refinement for Compound A Form D
Empirical formula
C35 H44 CI F4 N7 06.50
Formula weight
778.22
Temperature
90(2) K
Wavelength
1.54184 Å
Crystal system
Monoclinic
Space group
I 2
Unit cell dimensions
a = 20.2510(3) Å
α = 90º.
b = 8.73850(10) Å
ß = 112.156(2)º.
c = 22.2870(3) Å
γ = 90º.
Volume
3652.76(10) Å3
Z
4
Density (calculated)
1.415 Mg/m3
Absorption coefficient
1.598 mm−1
F(000)
1632
Crystal size
0.200 × 0.120 × 0.100 mm3
Theta range for data collection
2.516 to 75.031º.
Index ranges
−24 <= h <= 24,
−9 <= k <= 10,
−27 <= k <= 27
Reflections collected
28840
Independent reflections
6849 [R(int) = 0.0256]
Completeness to theta = 67.000º
100.0 %
Absorption correction
Gaussian
Max. and min. transmission
1.000 and 0.671
Refinement method
Full-matrix least-squares on F2
Data/restraints/parameters
6849/1/509
Goodness-of-fit on F2
1.048
Final R indices [I>2sigma(I)]
R1 = 0.0320, wR2 = 0.0899
R indices (all data)
R1 = 0.0323, wR2 = 0.0902
Absolute structure parameter
−0.009(5)
Extinction coefficient
0.00030(8)
Largest diff. peak and hole
1.072 and −0.188 e.Å−3
TABLE 20
Atomic coordinates (×104)and equivalent isotropic displacement
parameters (Å2 × 103)for Compound A Form D. U(eq) is defined
as one third of the trace of the orthogonalized Uij tensor.
x
y
z
U(eq)
C(1)
3573(1)
5230(3)
6770(1)
23(1)
C(2)
3021(1)
5999(3)
6231(1)
23(1)
C(3)
2279(1)
5675(3)
5985(1)
25(1)
C(4)
1829(1)
6460(3)
5458(1)
25(1)
C(5)
2072(1)
7610(3)
5151(1)
23(1)
C(6)
2777(1)
7969(3)
5421(1)
23(1)
C(7)
3269(1)
7229(3)
5965(1)
22(1)
C(8)
4368(1)
7039(3)
6722(1)
23(1)
C(9)
3956(1)
3494(3)
7706(1)
31(1)
C(10)
4306(1)
1966(3)
7677(1)
32(1)
C(11)
3297(1)
1196(3)
6730(1)
30(1)
C(12)
2936(1)
2738(3)
6713(1)
28(1)
C(13)
3568(2)
3460(4)
8177(1)
37(1)
C(14)
3642(1)
−507(3)
7667(1)
30(1)
C(15)
4070(2)
−760(4)
8367(1)
40(1)
C(16)
4045(2)
−2070(4)
8646(2)
46(1)
C(17)
1622(1)
8320(3)
4514(1)
23(1)
C(18)
1326(1)
9766(3)
4430(1)
25(1)
C(19)
974(1)
10322(3)
3785(1)
27(1)
C(20)
917(1)
9355(3)
3286(1)
27(1)
C(21)
1231(1)
7892(3)
3405(1)
25(1)
C(22)
1350(1)
10762(3)
4983(1)
31(1)
C(23)
690(2)
11921(4)
3637(1)
38(1)
C(24)
5276(1)
8670(3)
6669(1)
27(1)
C(25)
6079(1)
8610(3)
6908(1)
29(1)
C(26)
6375(1)
9814(3)
6575(2)
36(1)
C(27)
6974(2)
8987(5)
6419(2)
34(1)
C(28)
6658(2)
7409(3)
6254(1)
36(1)
C(26A)
6375(1)
9814(3)
6575(2)
36(1)
C(27A)
6369(4)
9037(10)
6025(4)
36(2)
C(28A)
6658(2)
7409(3)
6254(1)
36(1)
C(29)
6818(1)
6274(3)
7315(1)
35(1)
C(30)
5218(1)
4019(3)
6244(1)
28(1)
C(31)
4551(2)
3104(3)
5891(1)
32(1)
C(32)
4066(1)
3634(3)
5219(1)
30(1)
C(33)
3427(2)
2568(3)
4943(1)
40(1)
C(34)
2995(2)
2726(4)
4220(2)
47(1)
C(35)
2497(1)
4066(3)
3987(1)
32(1)
N(1)
3952(1)
7773(3)
6207(1)
24(1)
N(2)
4228(1)
5819(2)
7016(1)
24(1)
N(3)
3458(1)
3928(3)
7051(1)
27(1)
N(4)
3766(1)
794(3)
7388(1)
31(1)
N(5)
1585(1)
7400(2)
4018(1)
25(1)
N(6)
1200(1)
6941(3)
2921(1)
32(1)
N(7)
6321(1)
7079(3)
6737(1)
29(1)
O(1)
3181(1)
−1430(2)
7363(1)
39(1)
O(2)
5052(1)
7512(2)
7011(1)
26(1)
O(3)
5243(1)
5376(2)
6049(1)
33(1)
O(4)
5704(1)
3432(2)
6711(1)
39(1)
O(5)
2191(1)
4320(2)
3410(1)
38(1)
O(6)
2414(1)
4910(2)
4440(1)
35(1)
O(7)
5000
7215(5)
5000
84(2)
F(1)
3023(1)
9104(2)
5150(1)
32(1)
F(2)
696(1)
11166(2)
4942(1)
44(1)
F(3)
1665(1)
10118(2)
5567(1)
43(1)
F(4)
1703(1)
12087(2)
5009(1)
45(1)
Cl(1)
922(1)
6035(1)
5145(1)
34(1)
TABLE 21
Bond lengths [Å] and angles [°] for Compound A Form D.
C(1)—N(2)
1.332(3)
C(14)—O(1)
1.227(4)
C(1)—N(3)
1.361(3)
C(14)—N(4)
1.365(3)
C(1)—C(2)
1.461(3)
C(14)—C(15)
1.487(4)
C(2)—C(7)
1.409(3)
C(15)—C(16)
1.312(4)
C(2)—C(3)
1.419(3)
C(15)—H(15)
0.9500
C(3)—C(4)
1.368(3)
C(16)—H(16A)
0.9500
C(3)—H(3)
0.9500
C(16)—H(16B)
0.9500
C(4)—C(5)
1.404(3)
C(17)—N(5)
1.347(3)
C(4)—CI(1)
1.741(2)
C(17)—C(18)
1.381(3)
C(5)—C(6)
1.360(3)
C(18)—C(19)
1.428(3)
C(5)—C(17)
1.501(3)
C(18)—C(22)
1.494(3)
C(6)—F(1)
1.351(3)
C(19)—C(20)
1.367(4)
C(6)—C(7)
1.403(3)
C(19)—C(23)
1.499(4)
C(7)—N(1)
1.366(3)
C(20)—C(21)
1.408(4)
C(8)—N(1)
1.308(3)
C(20)—H(20)
0.9500
C(8)—N(2)
1.336(3)
C(21)—N(6)
1.344(3)
C(8)—O(2)
1.354(3)
C(21)—N(5)
1.351(3)
C(9)—N(3)
1.478(3)
C(22)—F(3)
1.337(3)
C(9)—C(10)
1.525(4)
C(22)—F(2)
1.339(3)
C(9)—C(13)
1.531 (3)
C(22)—F(4)
1.351(3)
C(9)—H(9)
1.0000
C(23)—H(23A)
0.9800
C(10)—N(4)
1.458(4)
C(23)—H(23B)
0.9800
C(10)—H(10A)
0.9900
C(23)—H(23C)
0.9800
C(10)—H(10B)
0.9900
C(24)—O(2)
1.438(3)
C(11)—N(4)
1.458(3)
C(24)—C(25)
1.509(3)
C(11)—C(12)
1.527(4)
C(24)—H(24A)
0.9900
C(11)—H(11A)
0.9900
C(24)—H(24B)
0.9900
C(11)—H(11B)
0.9900
C(25)—N(7)
1.521(4)
C(12)—N(3)
1.471(3)
C(25)—C(26)
1.533(4)
C(12)—H(12A)
0.9900
C(25)—C(26A)
1.533(4)
C(12)—H(12B)
0.9900
C(25)—H(25)
1.0000
C(13)—H(13A)
0.9800
C(26)—C(27)
1.560(5)
C(13)—H(13B)
0.9800
C(26)—H(26A)
0.9900
C(13)—H(13C)
0.9800
C(26)—H(26B)
0.9900
C(27)—C(28)
1.506(5)
N(6)—H(6A)
0.8800
C(27)—H(27A)
0.9900
N(6)—H(6B)
0.8800
C(27)—H(27B)
0.9900
N(7)—H(7)
1.0000
C(28)—N(7)
1.504(3)
O(6)—H(6)
0.8400
C(28)—H(28A)
0.9900
O(7)—H(7X)
1.05(7)
C(28)—H(28B)
0.9900
N(2)—C(1)—N(3)
116.8(2)
C(26A)—C(27A)
1.399(9)
N(2)—C(1)—C(2)
119.7(2)
C(26A)—H(26C)
0.9900
N(3)—C(1)—C(2)
123.5(2)
C(26A)—H(26D)
0.9900
C(7)—C(2)—C(3)
118.9(2)
C(27A)—C(28A)
1.550(9)
C(7)—C(2)—C(1)
114.4(2)
C(27A)—H(27C)
0.9900
C(3)—C(2)—C(1)
126.6(2)
C(27A)—H(27D)
0.9900
C(4)—C(3)—C(2)
119.8(2)
C(28A)—N(7)
1.504(3)
C(4)—C(3)—H(3)
120.1
C(28A)—H(28C)
0.9900
C(2)—C(3)—H(3)
120.1
C(28A)—H(28D)
0.9900
C(3)—C(4)—C(5)
122.3(2)
C(29)—N(7)
1.480(3)
C(3)—C(4)—CI(1)
119.84(18)
C(29)—H(29A)
0.9800
C(5)—C(4)—CI(1)
117.85(17)
C(29)—H(29B)
0.9800
C(6)—C(5)—C(4)
116.8(2)
C(29)—H(29C)
0.9800
C(6)—C(5)—C(17)
119.0(2)
C(30)—O(4)
1.241(3)
C(4)—C(5)—C(17)
123.8(2)
C(30)—O(3)
1.271(3)
F(1)—C(6)—C(5)
118.3(2)
C(30)—C(31)
1.511(4)
F(1)—C(6)—C(7)
117.51(19)
C(31)—C(32)
1.520(3)
C(5)—C(6)—C(7)
124.2(2)
C(31)—H(31A)
0.9900
N(1)—C(7)—C(6)
117.7(2)
C(31)—H(31B)
0.9900
N(1)—C(7)—C(2)
124.6(2)
C(32)—C(33)
1.523(4)
C(6)—C(7)—C(2)
117.7(2)
C(32)—H(32A)
0.9900
N(1)—C(8)—N(2)
129.6(2)
C(32)—H(32B)
0.9900
N(1)—C(8)—O(2)
118.1(2)
C(33)—C(34)
1.523(4)
N(2)—C(8)—O(2)
112.30(19)
C(33)—H(33A)
0.9900
N(3)—C(9)—C(10)
109.7(2)
C(33)—H(33B)
0.9900
N(3)—C(9)—C(13)
110.3(2)
C(34)—C(35)
1.504(4)
C(10)—C(9)—C(13)
112.3(2)
C(34)—H(34A)
0.9900
N(3)—C(9)—H(9)
108.1
C(34)—H(34B)
0.9900
C(10)—C(9)—H(9)
108.1
C(35)—O(5)
1.219(3)
C(13)—C(9)—H(9)
108.1
C(35)—O(6)
1.312(3)
N(4)—C(10)—C(9)
110.5(2)
N(4)—C(10)—H(10A)
109.5
C(17)—C(18)—C(22)
123.0(2)
C(9)—C(10)—H(10A)
109.5
C(19)—C(18)—C(22)
118.8(2)
N(4)—C(10)—H(10B)
109.5
C(20)—C(19)—C(18)
117.8(2)
C(9)—C(10)—H(10B)
109.5
C(20)—C(19)—C(23)
119.3(2)
H(10A)—C(10)—H(10B)
108.1
C(18)—C(19)—C(23)
122.9(2)
N(4)—C(11)—C(12)
111.2(2)
C(19)—C(20)—C(21)
120.9(2)
N(4)—C(11)—H(11A)
109.4
C(19)—C(20)—H(20)
119.5
C(12)—C(11)—H(11A)
109.4
C(21)—C(20)—H(20)
119.5
N(4)—C(11)—H(11B)
109.4
N(6)—C(21)—N(5)
117.5(2)
C(12)—C(11)—H(11B)
109.4
N(6)—C(21)—C(20)
121.9(2)
H(11A)—C(11)—H(11B)
108.0
N(5)—C(21)—C(20)
120.6(2)
N(3)—C(12)—C(11)
111.5(2)
F(3)—C(22)—F(2)
105.9(2)
N(3)—C(12)—H(12A)
109.3
F(3)—C(22)—F(4)
105.6(2)
C(11)—C(12)—H(12A)
109.3
F(2)—C(22)—F(4)
105.7(2)
N(3)—C(12)—H(12B)
109.3
F(3)—C(22)—C(18)
114.3(2)
C(11)—C(12)—H(12B)
109.3
F(2)—C(22)—C(18)
112.0(2)
H(12A)—C(12)—H(12B)
108.0
F(4)—C(22)—C(18)
112.8(2)
C(9)—C(13)—H(13A)
109.5
C(19)—C(23)—H(23A)
109.5
C(9)—C(13)—H(13B)
109.5
C(19)—C(23)—H(23B)
109.5
H(13A)—C(13)—H(13B)
109.5
H(23A)—C(23)—H(23B)
109.5
C(9)—C(13)—H(13C)
109.5
C(19)—C(23)—H(23C)
109.5
H(13A)—C(13)—H(13C)
109.5
H(23A)—C(23)—H(23C)
109.5
H(13B)—C(13)—H(13C)
109.5
H(23B)—C(23)—H(23C)
109.5
O(1)—C(14)—N(4)
121.9(2)
O(2)—C(24)—C(25)
107.61(19)
O(1)—C(14)—C(15)
120.2(3)
O(2)—C(24)—H(24A)
110.2
N(4)—C(14)—C(15)
117.9(3)
C(25)—C(24)—H(24A)
110.2
C(16)—C(15)—C(14)
120.9(3)
O(2)—C(24)—H(24B)
110.2
C(16)—C(15)—H(15)
119.5
C(25)—C(24)—H(24B)
110.2
C(14)—C(15)—H(15)
119.5
H(24A)—C(24)—H(24B)
108.5
C(15)—C(16)—H(16A)
120.0
C(24)—C(25)—N(7)
110.4(2)
C(15)—C(16)—H(16B)
120.0
C(24)—C(25)—C(26)
111.8(2)
H(16A)—C(16)—H(16B)
120.0
N(7)—C(25)—C(26)
105.2(2)
N(5)—C(17)—C(18)
123.3(2)
C(24)—C(25)—C(26A)
111.8(2)
N(5)—C(17)—C(5)
110.8(2)
N(7)—C(25)—C(26A)
105.2(2)
C(18)—C(17)—C(5)
125.7(2)
C(24)—C(25)—H(25)
109.8
C(17)—C(18)—C(19)
118.3(2)
N(7)—C(25)—H(25)
109.8
C(26)—C(25)—H(25)
109.8
H(28C)—C(28A)—H(28D)
109.3
C(25)—C(26)—C(27)
105.6(3)
N(7)—C(29)—H(29A)
109.5
C(25)—C(26)—H(26A)
110.6
N(7)—C(29)—H(29B)
109.5
C(27)—C(26)—H(26A)
110.6
H(29A)—C(29)—H(29B)
109.5
C(25)—C(26)—H(26B)
110.6
N(7)—C(29)—H(29C)
109.5
C(27)—C(26)—H(26B)
110.6
H(29A)—C(29)—H(29C)
109.5
H(26A)—C(26)—H(26B)
108.8
H(29B)—C(29)—H(29C)
109.5
C(28)—C(27)—C(26)
100.6(3)
O(4)—C(30)—O(3)
123.5(2)
C(28)—C(27)—H(27A)
111.6
O(4)—C(30)—C(31)
119.3(2)
C(26)—C(27)—H(27A)
111.6
O(3)—C(30)—C(31)
117.3(2)
C(28)—C(27)—H(27B)
111.6
C(30)—C(31)—C(32)
118.1(2)
C(26)—C(27)—H(27B)
111.6
C(30)—C(31)—H(31A)
107.8
H(27A)—C(27)—H(27B)
109.4
C(32)—C(31)—H(31A)
107.8
N(7)—C(28)—C(27)
105.4(2)
C(30)—C(31)—H(31B)
107.8
N(7)—C(28)—H(28A)
110.7
C(32)—C(31)—H(31B)
107.8
C(27)—C(28)—H(28A)
110.7
H(31A)—C(31)—H(31B)
107.1
N(7)—C(28)—H(28B)
110.7
C(31)—C(32)—C(33)
110.2(2)
C(27)—C(28)—H(28B)
110.7
C(31)—C(32)—H(32A)
109.6
H(28A)—C(28)—H(28B)
108.8
C(33)—C(32)—H(32A)
109.6
C(27A)—C(26A)—C(25)
102.4(4)
C(31)—C(32)—H(32B)
109.6
C(27A)—C(26A)—H(26C)
111.3
C(33)—C(32)—H(32B)
109.6
C(25)—C(26A)—H(26C)
111.3
H(32A)—C(32)—H(32B)
108.1
C(27A)—C(26A)—H(26D)
111.3
C(34)—C(33)—C(32)
115.7(3)
C(25)—C(26A)—H(26D)
111.3
C(34)—C(33)—H(33A)
108.4
H(26C)—C(26A)—H(26D)
109.2
C(32)—C(33)—H(33A)
108.4
C(26A)—C(27A)—C(28A)
106.2(5)
C(34)—C(33)—H(33B)
108.4
C(26A)—C(27A)—H(27C)
110.5
C(32)—C(33)—H(33B)
108.4
C(28A)—C(27A)—H(27C)
110.5
H(33A)—C(33)—H(33B)
107.4
C(26A)—C(27A)—H(27D)
110.5
C(35)—C(34)—C(33)
118.6(3)
C(28A)—C(27A)—H(27D)
110.5
C(35)—C(34)—H(34A)
107.7
H(27C)—C(27A)—H(27D)
108.7
C(33)—C(34)—H(34A)
107.7
N(7)—C(28A)—C(27A)
101.2(3)
C(35)—C(34)—H(34B)
107.7
N(7)—C(28A)—H(28C)
111.5
C(33)—C(34)—H(34B)
107.7
C(27A)—C(28A)—H(28C)
111.5
H(34A)—C(34)—H(34B)
107.1
N(7)—C(28A)—H(28D)
111.5
O(5)—C(35)—O(6)
123.2(2)
C(27A)—C(28A)—H(28D)
111.5
O(5)—C(35)—C(34)
121.0(2)
O(6)—C(35)—C(34)
115.8(2)
H(6A)—N(6)—H(6B)
120.0
C(8)—N(1)—C(7)
113.4(2)
C(29)—N(7)—C(28A)
111.8(2)
C(1)—N(2)—C(8)
117.93(19)
C(29)—N(7)—C(28)
111.8(2)
C(1)—N(3)—C(12)
124.79(19)
C(29)—N(7)—C(25)
112.2(2)
C(1)—N(3)—C(9)
119.8(2)
C(28A)—N(7)—C(25)
106.6(2)
C(12)—N(3)—C(9)
114.6(2)
C(28)—N(7)—C(25)
106.6(2)
C(14)—N(4)—C(11)
119.8(2)
C(29)—N(7)—H(7)
108.7
C(14)—N(4)—C(10)
128.3(2)
C(28)—N(7)—H(7)
108.7
C(11)—N(4)—C(10)
111.7(2)
C(25)—N(7)—H(7)
108.7
C(17)—N(5)—C(21)
119.0(2)
C(8)—O(2)—C(24)
115.77(17)
C(21)—N(6)—H(6A)
120.0
C(35)—O(6)—H(6)
109.5
C(21)—N(6)—H(6B)
120.0
H(6A)—N(6)—H(6B)
120.0
TABLE 22
Anisotropic displacement parameters (Å2 × 103)for Compound A
Form D. The anisotropic displacement factor exponent takes the
form: −2π2[h2a*2U11 + . . . + 2 h k a* b* U12].
U11
U22
U33
U23
U13
U12
C(1)
25(1)
26(1)
18(1)
0(1)
7(1)
1(1)
C(2)
23(1)
26(1)
19(1)
2(1)
7(1)
3(1)
C(3)
25(1)
28(1)
23(1)
2(1)
11(1)
−1(1)
C(4)
21(1)
31(1)
23(1)
−1(1)
9(1)
1(1)
C(5)
23(1)
26(1)
18(1)
0(1)
6(1)
3(1)
C(6)
23(1)
24(1)
21(1)
4(1)
7(1)
−1(1)
C(7)
21(1)
24(1)
19(1)
0(1)
6(1)
1(1)
C(8)
21(1)
25(1)
20(1)
1(1)
5(1)
0(1)
C(9)
32(1)
33(1)
22(1)
8(1)
4(1)
−3(1)
C(10)
27(1)
39(2)
27(1)
10(1)
7(1)
2(1)
C(11)
33(1)
31(1)
25(1)
4(1)
9(1)
0(1)
C(12)
26(1)
28(1)
26(1)
4(1)
7(1)
−3(1)
C(13)
47(2)
39(2)
25(1)
5(1)
12(1)
2(1)
C(14)
35(1)
28(1)
33(1)
6(1)
19(1)
9(1)
C(15)
43(2)
42(2)
37(1)
10(1)
18(1)
8(1)
C(16)
43(2)
51(2)
50(2)
23(1)
24(1)
15(1)
C(17)
19(1)
28(1)
20(1)
2(1)
6(1)
1(1)
C(18)
22(1)
31(1)
21(1)
2(1)
5(1)
4(1)
C(19)
21(1)
34(1)
24(1)
3(1)
5(1)
4(1)
C(20)
23(1)
35(1)
20(1)
4(1)
3(1)
3(1)
C(21)
23(1)
31(1)
21(1)
1(1)
7(1)
−1(1)
C(22)
27(1)
37(2)
24(1)
1(1)
6(1)
9(1)
C(23)
42(2)
37(2)
27(1)
4(1)
5(1)
14(1)
C(24)
22(1)
27(1)
29(1)
5(1)
5(1)
−2(1)
C(25)
25(1)
29(1)
29(1)
−1(1)
4(1)
−2(1)
C(26)
29(1)
30(2)
48(2)
2(1)
13(1)
−3(1)
C(27)
30(2)
35(2)
37(2)
−2(2)
13(2)
−2(2)
C(28)
41(1)
34(2)
34(1)
−1(1)
16(1)
−3(1)
C(26A)
29(1)
30(2)
48(2)
2(1)
13(1)
−3(1)
C(27A)
42(5)
33(5)
41(5)
1(3)
24(4)
−5(3)
C(28A)
41(1)
34(2)
34(1)
−1(1)
16(1)
−3(1)
C(29)
33(1)
34(2)
32(1)
3(1)
5(1)
4(1)
C(30)
35(1)
27(1)
23(1)
2(1)
11(1)
2(1)
C(31)
35(1)
26(1)
31(1)
3(1)
8(1)
−1(1)
C(32)
31(1)
25(1)
31(1)
1(1)
8(1)
−1(1)
C(33)
35(1)
27(1)
46(2)
2(1)
1(1)
−1(1)
C(34)
38(2)
36(2)
48(2)
−17(1)
−6(1)
6(1)
C(35)
27(1)
31(1)
32(1)
−6(1)
4(1)
0(1)
N(1)
20(1)
28(1)
21(1)
4(1)
4(1)
0(1)
N(2)
23(1)
27(1)
19(1)
3(1)
5(1)
1(1)
N(3)
29(1)
28(1)
20(1)
6(1)
3(1)
−3(1)
N(4)
33(1)
31(1)
28(1)
7(1)
9(1)
1(1)
N(5)
22(1)
30(1)
20(1)
1(1)
4(1)
2(1)
N(6)
35(1)
36(1)
20(1)
−1(1)
4(1)
7(1)
N(7)
26(1)
28(1)
28(1)
2(1
5(1)
−1(1)
O(1)
45(1)
32(1)
44(1)
6(1)
20(1)
−2(1)
O(2)
22(1)
29(1)
21(1)
4(1)
3(1)
−2(1)
O(3)
36(1)
27(1)
28(1)
2(1)
4(1)
−5(1)
O(4)
41(1)
37(1)
28(1)
3(1)
1(1)
4(1)
O(5)
37(1)
41(1)
29(1)
−8(1)
5(1)
6(1)
O(6)
40(1)
35(1)
27(1)
−2(1)
7(1)
10(1)
O(7)
160(5)
47(2)
28(2)
0
17(2)
0
F(1)
25(1)
34(1)
30(1)
14(1)
3(1)
−4(1)
F(2)
32(1)
63(1)
34(1)
−11(1)
11(1)
16(1)
F(3)
58(1)
45(1)
19(1)
1(1)
8(1)
22(1)
F(4)
53(1)
36(1)
42(1)
−11(1)
15(1)
−6(1)
Cl(1)
19(1)
48(1)
33(1)
10(1)
6(1)
−2(1)
TABLE 23
Hydrogen coordinates (×104) and isotropic displacement
parameters (Å2 × 103) for Compound A Form D.
x
y
z
U(eq)
H(3)
2096
4916
6185
30
H(9)
4338
4290
7859
37
H(10A)
4606
2079
7417
38
H(10B)
4618
1649
8120
38
H(11A)
2929
394
6556
36
H(11B)
3578
1242
6450
36
H(12A)
2677
3049
6257
33
H(12B)
2583
2634
6920
33
H(13A)
3335
4448
8166
56
H(13B)
3912
3264
8617
56
H(13C)
3208
2647
8050
56
H(15)
4366
39
8616
47
H(16A)
3751
−2873
8400
55
H(16B)
4322
−2215
9093
55
H(20)
661
9674
2852
33
H(23A)
1089
12646
3764
56
H(23B)
385
12144
3879
56
H(23C)
411
12017
3172
56
H(24A)
5119
9692
6754
33
H(24B)
5065
8475
6197
33
H(25)
6289
8764
7388
35
H(26A)
6572
10697
6866
43
H(26B)
5996
10186
6173
43
H(27A)
7049
9467
6048
41
H(27B)
7430
8971
6799
41
H(28A)
6296
7382
5806
43
H(28B)
7034
6648
6291
43
H(26C)
6066
10732
6456
43
H(26D)
6864
10125
6856
43
H(27C)
6677
9566
5835
43
H(27D)
5879
8983
5694
43
H(28C)
6502
6667
5891
43
H(28D)
7185
7400
6460
13
H(29A)
6941
5275
7187
53
H(29B)
6590
6129
7629
53
H(29C)
7252
6885
7513
53
H(31A)
4265
3079
6166
38
H(31B)
4696
2038
5853
38
H(32A)
4335
3644
4929
36
H(32B)
3899
4688
5244
36
H(33A)
3598
1500
5032
48
H(33B)
3105
2753
5178
48
H(34A)
3335
2762
3997
56
H(34B)
2709
1781
4074
56
H(6A)
1406
6037
3009
39
H(6B)
974
7223
2516
39
H(7)
5892
6419
6525
34
H(6)
2113
5599
4268
53
H(7X)
4400
5674
5035
101
H(7X)
4950(40)
6470(80)
5350(30)
110(20)
TABLE 24
Torsion angles [°] for Compound A Form D.
N(2)—C(1)—C(2)—C(7)
7.6(3)
N(3)—C(1)—C(2)—C(7)
−173.2(2)
N(2)—C(1)—C(2)—C(3)
−168.9(2)
N(3)—C(1)—C(2)—C(3)
10.2(4)
C(7)—C(2)—C(3)—C(4)
6.1(3)
C(1)—C(2)—C(3)—C(4)
−177.5(2)
C(2)—C(3)—C(4)—C(5)
−1.1(4)
C(2)—C(3)—C(4)—Cl(1)
178.61(18)
C(3)—C(4)—C(5)—C(6)
−3.2(3)
Cl(1)—C(4)—C(5)—C(6)
177.16(18)
C(3)—C(4)—C(5)—C(17)
169.9(2)
Cl(1)—C(4)—C(5)—C(17)
−9.8(3)
C(4)—C(5)—C(6)—F(1)
−177.9(2)
C(17)—C(5)—C(6)—F(1)
8.7(3)
C(4)—C(5)—C(6)—C(7)
2.4(3)
C(17)—C(5)—C(6)—C(7)
−171.0(2)
F(1)—C(6)—C(7)—N(1)
4.2(3)
C(5)—C(6)—C(7)—N(1)
−176.1(2)
F(1)—C(6)—C(7)—C(2)
−177.2(2)
C(5)—C(6)—C(7)—C(2)
2.5(3)
C(3)—C(2)—C(7)—N(1)
171.8(2)
C(1)—C(2)—C(7)—N(1)
−5.0(3)
C(3)—C(2)—C(7)—C(6)
−6.7(3)
C(1)—C(2)—C(7)—C(6)
176.5(2)
N(3)—C(9)—C(10)—N(4)
−55.9(3)
C(13)—C(9)—C(10)—N(4)
67.1(3)
N(4)—C(11)—C(12)—N(3)
50.9(3)
O(1)—C(14)—C(15)—C(16)
10.9(4)
N(4)—C(14)—C(15)—C(16)
−171.1(3)
C(6)—C(5)—C(17)—N(5)
93.6(3)
C(4)—C(5)—C(17)—N(5)
−79.2(3)
C(6)—C(5)—C(17)—C(18)
−81.4(3)
C(4)—C(5)—C(17)—C(18)
105.7(3)
N(5)—C(17)—C(18)—C(19)
−0.9(3)
C(5)—C(17)—C(18)—C(19)
173.5(2)
N(5)—C(17)—C(18)—C(22)
178.1(2)
C(5)—C(17)—C(18)—C(22)
−7.4(4)
C(17)—C(18)—C(19)—C(20)
3.4(3)
C(22)—C(18)—C(19)—C(20)
−175.7(2)
C(17)—C(18)—C(19)—C(23)
−174.6(2)
C(22)—C(18)—C(19)—C(23)
6.3(4)
C(18)—C(19)—C(20)—C(21)
−3.6(4)
C(23)—C(19)—C(20)—C(21)
174.4(2)
C(19)—C(20)—C(21)—N(6)
−177.9(2)
C(19)—C(20)—C(21)—N(5)
1.3(4)
C(17)—C(18)—C(22)—F(3)
−1.7(3)
C(19)—C(18)—C(22)—F(3)
177.4(2)
C(17)—C(18)—C(22)—F(2)
−122.1(2)
C(19)—C(18)—C(22)—F(2)
56.9(3)
C(17)—C(18)—C(22)—F(4)
118.9(2)
C(19)—C(18)—C(22)—F(4)
−62.0(3)
O(2)—C(24)—C(25)—N(7)
63.7(2)
O(2)—C(24)—C(25)—C(26)
−179.6(2)
O(2)—C(24)—C(25)—C(26A)
−179.6(2)
C(24)—C(25)—C(26)—C(27)
−137.9(3)
N(7)—C(25)—C(26)—C(27)
−18.1(3)
C(25)—C(26)—C(27)—C(28)
35.9(3)
C(26)—C(27)—C(28)—N(7)
−40.4(3)
C(24)—C(25)—C(26A)—C(27A)
−88.5(4)
N(7)—C(25)—C(26A)—C(27A)
31.3(4)
C(25)—C(26A)—C(27A)—C(28A)
−43.3(5)
C(26A)—C(27A)—C(28A)—N(7)
38.8(5)
O(4)—C(30)—C(31)—C(32)
−162.5(2)
O(3)—C(30)—C(31)—C(32)
18.5(3)
C(30)—C(31)—C(32)—C(33)
179.9(2)
C(31)—C(32)—C(33)—C(34)
−165.8(2)
C(32)—C(33)—C(34)—C(35)
−76.3(4)
C(33)—C(34)—C(35)—O(5)
173.2(3)
C(33)—C(34)—C(35)—O(6)
−7.6(4)
N(2)—C(8)—N(1)—C(7)
3.4(4)
O(2)—C(8)—N(1)—C(7)
−178.41(19)
C(6)—C(7)—N(1)—C(8)
178.4(2)
C(2)—C(7)—N(1)—C(8)
−0.1(3)
N(3)—C(1)—N(2)—C(8)
175.6(2)
C(2)—C(1)—N(2)—C(8)
−5.2(3)
N(1)—C(8)—N(2)—C(1)
−0.7(4)
O(2)—C(8)—N(2)—C(1)
−178.91(19)
N(2)—C(1)—N(3)—C(12)
−150.4(2)
C(2)—C(1)—N(3)—C(12)
30.4(3)
N(2)—C(1)—N(3)—C(9)
18.5(3)
C(2)—C(1)—N(3)—C(9)
−160.7(2)
C(11)—C(12)—N(3)—C(1)
119.6(2)
C(11)—C(12)—N(3)—C(9)
−49.9(3)
C(10)—C(9)—N(3)—C(1)
−117.9(2)
C(13)—C(9)—N(3)—C(1)
117.9(3)
C(10)—C(9)—N(3)—C(12)
52.1(3)
C(13)—C(9)—N(3)—C(12)
−72.1(3)
O(1)—C(14)—N(4)—C(11)
6.3(4)
C(15)—C(14)—N(4)—C(11)
171.7(2)
O(1)—C(14)—N(4)—C(10)
−177.8(2)
C(15)—C(14)—N(4)—C(10)
4.2(4)
C(12)—C(11)—N(4)—C(14)
119.4(2)
C(12)—C(11)—N(4)—C(10)
−57.1(3)
C(9)—C(10)—N(4)—C(14)
−116.2(3)
C(9)—C(10)—N(4)—C(11)
60.0(3)
C(18)—C(17)—N(5)—C(21)
−1.4(3)
C(5)—C(17)—N(5)—C(21)
−176.6(2)
N(6)—C(21)—N(5)—C(17)
−179.4(2)
C(20)—C(21)—N(5)—C(17)
1.3(3)
C(27A)—C(28A)—N(7)—C(29)
−140.1(4)
C(27A)—C(28A)—N(7)—C(25)
−17.2(4)
C(27)—C(28)—N(7)—C(29)
−92.4(3)
C(27)—C(28)—N(7)—C(25)
30.6(3)
C(24)—C(25)—N(7)—C(29)
−123.6(2)
C(26)—C(25)—N(7)—C(29)
115.7(2)
C(26A)—C(25)—N(7)—C(29)
115.7(2)
C(24)—C(25)—N(7)—C(28A)
113.7(2)
C(26A)—C(25)—N(7)—C(28A)
−7.0(2)
C(24)—C(25)—N(7)—C(28)
113.7(2)
C(26)—C(25)—N(7)—C(28)
−7.0(2)
N(1)—C(8)—O(2)—C(24)
−7.4(3)
N(2)—C(8)—O(2)—C(24)
171.03(19)
C(25)—C(24)—O(2)—C(8)
−158.6(2)
The single crystal structure of Compound A Form D is shown in FIG. 20. C6 and C25 of Compound A Form D are in the S configuration. The Flack [2] parameter for this structure is 0.007(8). For the inverted structure, with C6 and C25 in the R configuration the Flack parameter is 0.996(8). Determination of the absolute structure using Bayesian statistics on Bijvoet differences [3] reveals that the probability of the absolute structure as presented being correct is 1.000, while the probabilities of the absolute structure being a racemic twin or false are both 0.000. The Flack equivalent and its uncertainty are calculated through this program to be 0.011(6). The calculation was based on 3344 Bijvoet pairs with a coverage of 92%.
There are five intermolecular hydrogen bonds in the crystal structure of Form D. A water molecule (O7) sits on a 2-fold axis and is hydrogen bonded to two symmetry related carbonyl oxygen atoms (O4). The carboxylic group of the adipate forms a heterodimer through the O—H . . . N and O . . . H—N intramolecular interactions with nitrogen N5 and N6 of the API molecule. Anime nitrogen atom N6 is also involved in a hydrogen bond interaction to oxygen O3 of the adipate. Additionally, nitrogen N7 of disordered 1-methylpyrrolidine is involved in one N—H . . . O intermolecular interaction to oxygen O4 of the —COO— group of adipate. Views of the crystal packing within the unit cell can be seen in FIG. 21 and FIG. 22. For clarity all hydrogen atoms have been removed from packing diagrams.
Overall Summary. Compound A was the most stable form for further development of Compound 1. The amorphous form is considered for development purposes to be unstable for further development. Not only is the adipate salt of Compound A far more stable than the other identified salt forms, but it is also useful in the crystallization and purification of the compound during large scale synthesis.
Example 6—Compound A Form C
X-ray quality crystals were grown from a saturated methylethylketone solution that was allowed to slowly evaporate under ambient conditions. A colorless prism 0.170×0.080×0.060 mm in size was mounted on a Cryoloop with Paratone oil. Data were collected in a nitrogen gas stream at 90(2) K using phi and omega scans. Crystal-to-detector distance was 40 mm and exposure time was 0.05 seconds per frame using a scan width of 0.5°. Data collection was 100.0% complete to 67.000° in θ. A total of 43859 reflections were collected covering the indices, −25<=h<=25, −10<=k<=10, −27<=l<=27. 7083 reflections were found to be symmetry independent, with an Rint of 0.0360. Indexing and unit cell refinement indicated an I-centered, monoclinic lattice. The space group was found to be l 2 (No. 5). The data were integrated and scaled using CrysAlisPro 1.171.41.76a. Solution by iterative methods (SHELXT-2014) produced a complete heavy-atom phasing model. All non-hydrogen atoms were refined anisotropically by full-matrix least-squares (SHELXL-2018). All hydrogen atoms were placed using a riding model. Their positions were constrained relative to their parent atom using the appropriate HFIX command in SHELXL-2018.
TABLE 25
Hydrogen bond information for Form C
D—H . . . A
d(D—H)
d(H . . . A)
d(D . . . A)
<(DHA)
N6—H6B . . . O5
0.85(7)
2.13(7)
2.976(8)
175(5)
N6—H6A . . . O3#1
0.90(7)
1.96(7)
2.799(8)
156(6)
N6—H6A . . . O3A#1
0.90(7)
1.95(7)
2.800(10)
158(6)
O6—H6C . . . N5
0.84
1.85
2.662(6)
163.2
N7A—H7A . . . O4A#2
1.00
1.58
2.559(13)
163.5
N7—H7 . . . O4
1.00
1.64
2.62(2)
166.2
#1 x + 1/2, y + 1/2, z + 1/2
#2 x, y + 1, z
TABLE 26
Crystal data and structure refinement for Compound A Form C
Empirical formula
C35 H42 Cl F4 N7 O6
Formula weight
768.20
Temperature
90(2) K
Wavelength
1.54184 Å
Crystal system
Monoclinic
Space group
I 2
Unit cell dimensions
a = 20.4022(2) Å
α = 90°.
b = 8.63050(10) Å
β = 113.7020(10)°.
c = 22.3422(3) Å
γ = 90°.
Volume
3602.20(8) Å3
Z
4
Density (calculated)
1.417 Mg/m3
Absorption coefficient
1.604 mm−1
F(000)
1608
Crystal size
0.170 × 0.080 × 0.060 mm3
Theta range for data
2.480 to 75.125°.
collection
Index ranges
−25 <= h <= 25, −10 <= k <= 10,
−27 <= k <= 27
Reflections collected
43859
Independent reflections
7083 [R(int) = 0.0360]
Completeness to
100.0%
theta = 67.000°
Absorption correction
Gaussian
Max. and min.
1.000 and 0.678
transmission
Refinement method
Full-matrix least-squares on F2
Data/restraints/
7083/1/574
parameters
Goodness-of-fit on F2
1.082
Final R indices
R1 = 0.0333, wR2 = 0.0862
[I > 2sigma(I)]
R indices (all data)
R1 = 0.0337, wR2 = 0.0864
Absolute structure
0.009(5)
parameter
Extinction coefficient
0.00053(7)
Largest diff. peak and
0.211 and −0.190 e.Å−3
hole
TABLE 27
Atomic coordinates (×104) and equivalent isotropic displacement
parameters (Å2 × 103) for Compound A Form C. U(eq) is defined
as one third of the trace of the orthogonalized Uij tensor.
x
y
z
U(eq)
C(1)
3569(1)
5187(3)
6766(1)
28(1)
C(2)
3022(1)
5959(3)
6211(1)
27(1)
C(3)
2277(1)
5656(3)
5958(1)
29(1)
C(4)
1824(1)
6453(3)
5424(1)
30(1)
C(5)
2064(1)
7612(3)
5116(1)
30(1)
C(6)
2781(1)
7942(3)
5392(1)
32(1)
C(7)
3277(1)
7176(3)
5942(1)
29(1)
C(8)
4381(1)
6963(3)
6725(1)
29(1)
C(9)
2944(1)
2666(3)
6687(1)
35(1)
C(10)
3349(2)
1165(4)
6713(1)
40(1)
C(11)
4321(2)
1985(4)
7702(1)
38(1)
C(12)
3936(2)
3479(4)
7725(1)
37(1)
C(13)
3534(2)
3353(5)
8168(2)
51(1)
C(14)
3665(2)
−542(4)
7659(2)
39(1)
C(15)
4067(2)
−775(4)
8372(2)
48(1)
C(16)
4021(2)
−2091(5)
8648(2)
56(1)
C(17)
1612(1)
8368(3)
4481(1)
29(1)
C(18)
1315(1)
9823(3)
4409(1)
31(1)
C(19)
966(1)
10437(4)
3766(1)
33(1)
C(20)
914(1)
9507(3)
3251(1)
33(1)
C(21)
1218(1)
8023(3)
3356(1)
30(1)
C(22)
1342(2)
10781(4)
4979(1)
38(1)
C(23)
685(2)
12064(4)
3633(2)
46(1)
C(24)
5314(1)
8584(4)
6710(1)
37(1)
C(25)
6106(3)
8603(6)
6915(2)
28(1)
C(26)
6685(3)
7468(7)
6261(3)
38(1)
C(27)
7039(8)
9033(17)
6491(8)
48(3)
C(28)
6404(3)
9875(7)
6613(3)
34(1)
C(29)
6845(3)
6234(7)
7308(3)
36(1)
C(30)
5223(3)
4190(6)
6172(2)
29(1)
C(31)
4575(2)
3362(5)
5781(2)
61(1)
C(24A)
5314(1)
8584(4)
6710(1)
37(1)
C(25A)
5580(3)
7619(6)
6293(3)
32(1)
C(26A)
6541(4)
9165(9)
6316(5)
44(2)
C(27A)
6865(3)
7775(8)
6773(3)
43(1)
C(28A)
6236(10)
6689(19)
6628(9)
38(3)
C(29A)
5735(4)
8081(8)
5271(3)
44(1)
C(24X)
5314(1)
8584(4)
6710(1)
37(1)
C(25X)
6106(3)
8603(6)
6915(2)
28(1)
C(26X)
6685(3)
7468(7)
6261(3)
38(1)
C(27X)
6359(8)
9077(16)
5978(7)
35(3)
C(28X)
6404(3)
9875(7)
6613(3)
34(1)
C(29X)
6845(3)
6234(7)
7308(3)
36(1)
C(30A)
5080(4)
2199(7)
5921(3)
43(1)
C(31A)
4575(2)
3362(5)
5781(2)
61(1)
C(32)
4027(2)
3718(4)
5108(2)
49(1)
C(33)
3397(2)
2605(4)
4900(2)
43(1)
C(34)
2910(2)
2681(5)
4181(2)
63(1)
C(35)
2454(2)
4099(4)
3935(2)
48(1)
N(1)
3972(1)
7681(3)
6192(1)
32(1)
N(2)
4233(1)
5756(3)
7026(1)
29(1)
N(3)
3436(1)
3900(3)
7054(1)
34(1)
N(4)
3806(1)
759(3)
7383(1)
38(1)
N(5)
1573(1)
7475(3)
3971(1)
29(1)
N(6)
1184(1)
7084(3)
2865(1)
38(1)
N(7)
6365(8)
7098(15)
6742(7)
35(2)
N(7A)
5795(3)
8759(6)
5901(2)
34(1)
N(7X)
6365(8)
7098(15)
6742(7)
35(2)
O(1)
3208(1)
−1477(3)
7332(1)
48(1)
O(2)
5072(1)
7420(2)
7032(1)
34(1)
O(3)
5233(2)
5533(4)
5952(2)
35(1)
O(4)
5711(2)
3642(5)
6664(2)
39(1)
O(3A)
4993(2)
1157(5)
5494(2)
43(1)
O(4A)
5551(3)
2146(6)
6493(2)
62(1)
O(5)
2368(2)
4928(3)
4384(1)
54(1)
O(6)
2169(1)
4400(3)
3354(1)
60(1)
F(1)
3028(1)
9071(2)
5121(1)
45(1)
F(2)
1703(1)
12108(2)
5040(1)
54(1)
F(3)
682(1)
11204(3)
4915(1)
56(1)
F(4)
1643(1)
10074(2)
5554(1)
53(1)
Cl(1)
906(1)
6064(1)
5100(1)
38(1)
TABLE 28
Bond lengths [A] and angles [°] for Compound A Form C.
C(1)—N(2)
1.334(3)
C(14)—C(15)
1.482(4)
C(1)—N(3)
1.364(4)
C(15)—C(16)
1.315(5)
C(1)—C(2)
1.455(3)
C(15)—H(15)
0.9500
C(2)—C(7)
1.410(4)
C(16)—H(16A)
0.9500
C(2)—C(3)
1.416(3)
C(16)—H(16B)
0.9500
C(3)—C(4)
1.365(4)
C(17)—N(5)
1.352(3)
C(3)—H(3)
0.9500
C(17)—C(18)
1.375(4)
C(4)—C(5)
1.409(4)
C(18)—C(19)
1.425(4)
C(4)—Cl(1)
1.747(3)
C(18)—C(22)
1.501(4)
C(5)—C(6)
1.369(4)
C(19)—C(20)
1.370(4)
C(5)—C(17)
1.496(3)
C(19)—C(23)
1.500(4)
C(6)—F(1)
1.348(3)
C(20)—C(21)
1.401(4)
C(6)—C(7)
1.404(4)
C(20)—H(20)
0.9500
C(7)—N(1)
1.368(3)
C(21)—N(6)
1.344(4)
C(8)—N(1)
1.303(3)
C(21)—N(5)
1.355(3)
C(8)—N(2)
1.340(4)
C(22)—F(4)
1.329(3)
C(8)—O(2)
1.354(3)
C(22)—F(2)
1.339(4)
C(9)—N(3)
1.467(4)
C(22)—F(3)
1.347(3)
C(9)—C(10)
1.525(4)
C(23)—H(23A)
0.9800
C(9)—H(9A)
0.9900
C(23)—H(23B)
0.9800
C(9)—H(9B)
0.9900
C(23)—H(23C)
0.9800
C(10)—N(4)
1.452(3)
C(24)—O(2)
1.434(4)
C(10)—H(10A)
0.9900
C(24)—C(25)
1.491(5)
C(10)—H(10B)
0.9900
C(24)—H(24A)
0.9900
C(11)—N(4)
1.460(4)
C(24)—H(24B)
0.9900
C(11)—C(12)
1.521(4)
C(25)—N(7)
1.510(15)
C(11)—H(11A)
0.9900
C(25)—C(28)
1.537(8)
C(11)—H(11B)
0.9900
C(25)—H(25)
1.0000
C(12)—N(3)
1.480(3)
C(26)—N(7)
1.499(17)
C(12)—C(13)
1.522(4)
C(26)—C(27)
1.521(18)
C(12)—H(12)
1.0000
C(26)—H(26A)
0.9900
C(13)—H(13A)
0.9800
C(26)—H(26B)
0.9900
C(13)—H(13B)
0.9800
C(27)—C(28)
1.603(14)
C(13)—H(13C)
0.9800
C(27)—H(27A)
0.9900
C(14)—O(1)
1.228(4)
C(27)—H(27B)
0.9900
C(14)—N(4)
1.366(4)
C(28)—H(28A)
0.9900
C(28)—H(28B)
0.9900
C(25X)—C(28X)
1.537(8)
C(29)—N(7)
1.456(17)
C(25X)—H(25X)
1.0000
C(29)—H(29A)
0.9800
C(26X)—N(7X)
1.499(17)
C(29)—H(29B)
0.9800
C(26X)—C(27X)
1.560(16)
C(29)—H(29C)
0.9800
C(26X)—H(26E)
0.9900
C(30)—O(4)
1.242(6)
C(26X)—H(26F)
0.9900
C(30)—O(3)
1.263(7)
C(27X)—C(28X)
1.546(14)
C(30)—C(31)
1.448(7)
C(27X)—H(27E)
0.9900
C(31)—C(32)
1.501(5)
C(27X)—H(27F)
0.9900
C(31)—H(31A)
0.9900
C(28X)—H(28E)
0.9900
C(31)—H(31B)
0.9900
C(28X)—H(28F)
0.9900
C(24A)—O(2)
1.434(4)
C(29X)—N(7X)
1.456(17)
C(24A)—C(25A)
1.504(6)
C(29X)—H(29G)
0.9800
C(24A)—H(24C)
0.9900
C(29X)—H(29H)
0.9800
C(24A)—H(24D)
0.9900
C(29X)—H(291)
0.9800
C(25A)—C(28A)
1.48(2)
C(30A)—O(4A)
1.253(8)
C(25A)—N(7A)
1.495(7)
C(30A)—O(3A)
1.271(8)
C(25A)—H(25A)
1.0000
C(30A)—C(31A)
1.383(8)
C(26A)—N(7A)
1.470(9)
C(31A)—C(32)
1.501(5)
C(26A)—C(27A)
1.542(10)
C(31A)—H(31C)
0.9900
C(26A)—H(26C)
0.9900
C(31A)—H(31D)
0.9900
C(26A)—H(26D)
0.9900
C(32)—C(33)
1.520(5)
C(27A)—C(28A)
1.516(15)
C(32)—H(32A)
0.9900
C(27A)—H(27C)
0.9900
C(32)—H(32B)
0.9900
C(27A)—H(27D)
0.9900
C(33)—C(34)
1.514(5)
C(28A)—H(28C)
0.9900
C(33)—H(33A)
0.9900
C(28A)—H(28D)
0.9900
C(33)—H(33B)
0.9900
C(29A)—N(7A)
1.482(8)
C(34)—C(35)
1.501(5)
C(29A)—H(29D)
0.9800
C(34)—H(34A)
0.9900
C(29A)—H(29E)
0.9800
C(34)—H(34B)
0.9900
C(29A)—H(29F)
0.9800
C(35)—O(6)
1.219(4)
C(24X)—O(2)
1.434(4)
C(35)—O(5)
1.300(4)
C(24X)—C(25X)
1.491(5)
N(6)—H(6A)
0.8800
C(24X)—H(24E)
0.9900
N(6)—H(6B)
0.8800
C(24X)—H(24F)
0.9900
N(7)—H(7)
1.0000
C(25X)—N(7X)
1.510(15)
N(7A)—H(7A)
1.0000
N(7X)—H(7X)
1.0000
C(9)—C(10)—H(10B)
109.4
O(5)—H(5)
0.8400
H(10A)—C(10)—H(10B)
108.0
N(2)—C(1)—N(3)
117.1(2)
N(4)—C(11)—C(12)
110.5(2)
N(2)—C(1)—C(2)
119.9(2)
N(4)—C(11)—H(11A)
109.5
N(3)—C(1)—C(2)
123.0(2)
C(12)—C(11)—H(11A)
109.5
C(7)—C(2)—C(3)
119.2(2)
N(4)—C(11)—H(11B)
109.5
C(7)—C(2)—C(1)
114.6(2)
C(12)—C(11)—H(11B)
109.5
C(3)—C(2)—C(1)
126.0(2)
H(11A)—C(11)—H(11B)
108.1
C(4)—C(3)—C(2)
119.9(2)
N(3)—C(12)—C(11)
109.2(2)
C(4)—C(3)—H(3)
120.1
N(3)—C(12)—C(13)
110.2(2)
C(2)—C(3)—H(3)
120.1
C(11)—C(12)—C(13)
112.4(3)
C(3)—C(4)—C(5)
122.5(2)
N(3)—C(12)—H(12)
108.3
C(3)—C(4)—Cl(1)
120.2(2)
C(11)—C(12)—H(12)
108.3
C(5)—C(4)—Cl(1)
117.35(19)
C(13)—C(12)—H(12)
108.3
C(6)—C(5)—C(4)
116.5(2)
C(12)—C(13)—H(13A)
109.5
C(6)—C(5)—C(17)
118.4(2)
C(12)—C(13)—H(13B)
109.5
C(4)—C(5)—C(17)
124.7(2)
H(13A)—C(13)—H(13B)
109.5
F(1)—C(6)—C(5)
118.2(2)
C(12)—C(13)—H(13C)
109.5
F(1)—C(6)—C(7)
117.7(2)
H(13A)—C(13)—H(13C)
109.5
C(5)—C(6)—C(7)
124.1(2)
H(13B)—C(13)—H(13C)
109.5
N(1)—C(7)—C(6)
118.2(2)
O(1)—C(14)—N(4)
121.2(3)
N(1)—C(7)—C(2)
124.2(2)
O(1)—C(14)—C(15)
120.7(3)
C(6)—C(7)—C(2)
117.6(2)
N(4)—C(14)—C(15)
118.1(3)
N(1)—C(8)—N(2)
129.5(2)
C(16)—C(15)—C(14)
120.6(4)
N(1)—C(8)—O(2)
118.6(2)
C(16)—C(15)—H(15)
119.7
N(2)—C(8)—O(2)
111.8(2)
C(14)—C(15)—H(15)
119.7
N(3)—C(9)—C(10)
110.9(2)
C(15)—C(16)—H(16A)
120.0
N(3)—C(9)—H(9A)
109.5
C(15)—C(16)—H(16B)
120.0
C(10)—C(9)—H(9A)
109.5
H(16A)—C(16)—H(16B)
120.0
N(3)—C(9)—H(9B)
109.5
N(5)—C(17)—C(18)
123.2(2)
C(10)—C(9)—H(9B)
109.5
N(5)—C(17)—C(5)
110.9(2)
H(9A)—C(9)—H(9B)
108.1
C(18)—C(17)—C(5)
125.8(2)
N(4)—C(10)—C(9)
110.9(2)
C(17)—C(18)—C(19)
118.4(2)
N(4)—C(10)—H(10A)
109.4
C(17)—C(18)—C(22)
122.6(2)
C(9)—C(10)—H(10A)
109.4
C(19)—C(18)—C(22)
119.0(3)
N(4)—C(10)—H(10B)
109.4
C(20)—C(19)—C(18)
117.9(3)
C(20)—C(19)—C(23)
119.2(2)
C(27)—C(26)—H(26B)
111.1
C(18)—C(19)—C(23)
122.9(3)
H(26A)—C(26)—H(26B)
109.0
C(19)—C(20)—C(21)
121.0(2)
C(26)—C(27)—C(28)
98.8(9)
C(19)—C(20)—H(20)
119.5
C(26)—C(27)—H(27A)
112.0
C(21)—C(20)—H(20)
119.5
C(28)—C(27)—H(27A)
112.0
N(6)—C(21)—N(5)
116.7(3)
C(26)—C(27)—H(27B)
112.0
N(6)—C(21)—C(20)
122.7(2)
C(28)—C(27)—H(27B)
112.0
N(5)—C(21)—C(20)
120.6(2)
H(27A)—C(27)—H(27B)
109.7
F(4)—C(22)—F(2)
105.8(2)
C(25)—C(28)—C(27)
103.9(7)
F(4)—C(22)—F(3)
106.3(2)
C(25)—C(28)—H(28A)
111.0
F(2)—C(22)—F(3)
105.4(3)
C(27)—C(28)—H(28A)
111.0
F(4)—C(22)—C(18)
114.4(3)
C(25)—C(28)—H(28B)
111.0
F(2)—C(22)—C(18)
112.9(2)
C(27)—C(28)—H(28B)
111.0
F(3)—C(22)—C(18)
111.4(2)
H(28A)—C(28)—H(28B)
109.0
C(19)—C(23)—H(23A)
109.5
N(7)—C(29)—H(29A)
109.5
C(19)—C(23)—H(23B)
109.5
N(7)—C(29)—H(29B)
109.5
H(23A)—C(23)—H(23B)
109.5
H(29A)—C(29)—H(29B)
109.5
C(19)—C(23)—H(23C)
109.5
N(7)—C(29)—H(29C)
109.5
H(23A)—C(23)—H(23C)
109.5
H(29A)—C(29)—H(29C)
109.5
H(23B)—C(23)—H(23C)
109.5
H(29B)—C(29)—H(29C)
109.5
O(2)—C(24)—C(25)
113.8(3)
O(4)—C(30)—O(3)
124.2(5)
O(2)—C(24)—H(24A)
108.8
O(4)—C(30)—C(31)
124.0(5)
C(25)—C(24)—H(24A)
108.8
O(3)—C(30)—C(31)
111.8(4)
O(2)—C(24)—H(24B)
108.8
C(30)—C(31)—C(32)
129.4(4)
C(25)—C(24)—H(24B)
108.8
C(30)—C(31)—H(31A)
104.9
H(24A)—C(24)—H(24B)
107.7
C(32)—C(31)—H(31A)
104.9
C(24)—C(25)—N(7)
111.0(6)
C(30)—C(31)—H(31B)
104.9
C(24)—C(25)—C(28)
116.3(4)
C(32)—C(31)—H(31B)
104.9
N(7)—C(25)—C(28)
105.1(7)
H(31A)—C(31)—H(31B)
105.8
C(24)—C(25)—H(25)
108.0
O(2)—C(24A)—C(25A)
101.9(3)
N(7)—C(25)—H(25)
108.0
O(2)—C(24A)—H(24C)
111.4
C(28)—C(25)—H(25)
108.0
C(25A)—C(24A)—H(24C)
111.4
N(7)—C(26)—C(27)
103.4(7)
O(2)—C(24A)—H(24D)
111.4
N(7)—C(26)—H(26A)
111.1
C(25A)—C(24A)—H(24D)
111.4
C(27)—C(26)—H(26A)
111.1
H(24C)—C(24A)—H(24D)
109.2
N(7)—C(26)—H(26B)
111.1
C(28A)—C(25A)—N(7A)
103.7(8)
C(28A)—C(25A)—C(24A)
117.6(8)
C(24X)—C(25X)—C(28X)
116.3(4)
N(7A)—C(25A)—C(24A)
105.2(4)
N(7X)—C(25X)—C(28X)
105.1(7)
C(28A)—C(25A)—H(25A)
110.0
C(24X)—C(25X)—H(25X)
108.0
N(7A)—C(25A)—H(25A)
110.0
N(7X)—C(25X)—H(25X)
108.0
C(24A)—C(25A)—H(25A)
110.0
C(28X)—C(25X)—H(25X)
108.0
N(7A)—C(26A)—C(27A)
107.0(5)
N(7X)—C(26X)—C(27X)
104.0(9)
N(7A)—C(26A)—H(26C)
110.3
N(7X)—C(26X)—H(26E)
110.9
C(27A)—C(26A)—H(26C)
110.3
C(27X)—C(26X)—H(26E)
110.9
N(7A)—C(26A)—H(26D)
110.3
N(7X)—C(26X)—H(26F)
110.9
C(27A)—C(26A)—H(26D)
110.3
C(27X)—C(26X)—H(26F)
110.9
H(26C)—C(26A)—H(26D)
108.6
H(26E)—C(26X)—H(26F)
109.0
C(28A)—C(27A)—C(26A)
103.8(9)
C(28X)—C(27X)—C(26X)
99.6(9)
C(28A)—C(27A)—H(27C)
111.0
C(28X)—C(27X)—H(27E)
111.9
C(26A)—C(27A)—H(27C)
111.0
C(26X)—C(27X)—H(27E)
111.9
C(28A)—C(27A)—H(27D)
111.0
C(28X)—C(27X)—H(27F)
111.9
C(26A)—C(27A)—H(27D)
111.0
C(26X)—C(27X)—H(27F)
111.9
H(27C)—C(27A)—H(27D)
109.0
H(27E)—C(27X)—H(27F)
109.6
C(25A)—C(28A)—C(27A)
106.7(11)
C(25X)—C(28X)—C(27X)
101.4(6)
C(25A)—C(28A)—H(28C)
110.4
C(25X)—C(28X)—H(28E)
111.5
C(27A)—C(28A)—H(28C)
110.4
C(27X)—C(28X)—H(28E)
111.5
C(25A)—C(28A)—H(28D)
110.4
C(25X)—C(28X)—H(28F)
111.5
C(27A)—C(28A)—H(28D)
110.4
C(27X)—C(28X)—H(28F)
111.5
H(28C)—C(28A)—H(28D)
108.6
H(28E)—C(28X)—H(28F)
109.3
N(7A)—C(29A)—H(29D)
109.5
N(7X)—C(29X)—H(29G)
109.5
N(7A)—C(29A)—H(29E)
109.5
N(7X)—C(29X)—H(29H)
109.5
H(29D)—C(29A)—H(29E)
109.5
H(29G)—C(29X)—H(29H)
109.5
N(7A)—C(29A)—H(29F)
109.5
N(7X)—C(29X)—H(291)
109.5
H(29D)—C(29A)—H(29F)
109.5
H(29G)—C(29X)—H(291)
109.5
H(29E)—C(29A)—H(29F)
109.5
H(29H)—C(29X)—H(291)
109.5
O(2)—C(24X)—C(25X)
113.8(3)
O(4A)—C(30A)—O(3A)
124.0(6)
O(2)—C(24X)—H(24E)
108.8
O(4A)—C(30A)—C(31A)
116.9(5)
C(25X)—C(24X)—H(24E)
108.8
O(3A)—C(30A)—C(31A)
118.5(6)
O(2)—C(24X)—H(24F)
108.8
C(30A)—C(31A)—C(32)
124.2(4)
C(25X)—C(24X)—H(24F)
108.8
C(30A)—C(31A)—H(31C)
106.3
H(24E)—C(24X)—H(24F)
107.7
C(32)—C(31A)—H(31C)
106.3
C(24X)—C(25X)—N(7X)
111.0(6)
C(30A)—C(31A)—H(31D)
106.3
C(32)—C(31A)—H(31D)
106.3
C(14)—N(4)—C(10)
120.0(3)
H(31C)—C(31A)—H(31D)
106.4
C(14)—N(4)—C(11)
128.0(2)
C(31A)—C(32)—C(33)
112.0(3)
C(10)—N(4)—C(11)
111.5(2)
C(31)—C(32)—C(33)
112.0(3)
C(17)—N(5)—C(21)
118.8(2)
C(31)—C(32)—H(32A)
109.2
C(21)—N(6)—H(6A)
120.0
C(33)—C(32)—H(32A)
109.2
C(21)—N(6)—H(6B)
120.0
C(31)—C(32)—H(32B)
109.2
H(6A)—N(6)—H(6B)
120.0
C(33)—C(32)—H(32B)
109.2
C(29)—N(7)—C(26)
113.4(11)
H(32A)—C(32)—H(32B)
107.9
C(29)—N(7)—C(25)
113.6(9)
C(34)—C(33)—C(32)
114.3(3)
C(26)—N(7)—C(25)
107.4(9)
C(34)—C(33)—H(33A)
108.7
C(29)—N(7)—H(7)
107.4
C(32)—C(33)—H(33A)
108.7
C(26)—N(7)—H(7)
107.4
C(34)—C(33)—H(33B)
108.7
C(25)—N(7)—H(7)
107.4
C(32)—C(33)—H(33B)
108.7
C(26A)—N(7A)—C(29A)
111.2(6)
H(33A)—C(33)—H(33B)
107.6
C(26A)—N(7A)—C(25A)
105.0(5)
C(35)—C(34)—C(33)
118.0(3)
C(29A)—N(7A)—C(25A)
111.4(5)
C(35)—C(34)—H(34A)
107.8
C(26A)—N(7A)—H(7A)
109.7
C(33)—C(34)—H(34A)
107.8
C(29A)—N(7A)—H(7A)
109.7
C(35)—C(34)—H(34B)
107.8
C(25A)—N(7A)—H(7A)
109.7
C(33)—C(34)—H(34B)
107.8
C(29X)—N(7X)—C(26X)
113.4(11)
H(34A)—C(34)—H(34B)
107.1
C(29X)—N(7X)—C(25X)
113.6(9)
O(6)—C(35)—O(5)
123.4(3)
C(26X)—N(7X)—C(25X)
107.4(9)
O(6)—C(35)—C(34)
121.6(3)
C(29X)—N(7X)—H(7X)
107.4
O(5)—C(35)—C(34)
115.0(3)
C(26X)—N(7X)—H(7X)
107.4
C(8)—N(1)—C(7)
113.6(2)
C(25X)—N(7X)—H(7X)
107.4
C(1)—N(2)—C(8)
117.6(2)
C(8)—O(2)—C(24X)
116.7(2)
C(1)—N(3)—C(9)
123.3(2)
C(8)—O(2)—C(24)
116.7(2)
C(1)—N(3)—C(12)
119.4(2)
C(8)—O(2)—C(24A)
116.7(2)
C(9)—N(3)—C(12)
115.2(2)
C(35)—O(5)—H(5)
109.5
TABLE 29
Anisotropic displacement parameters (Å2 × 103)for Compound A
Form C. The anisotropic displacement factor exponent takes the
form: −2π2[h2a*2U11 + . . . + 2 h k a* b* U12].
U11
U22
U33
U23
U13
U12
C(1)
26(1)
36(1)
22(1)
−2(1)
9(1)
0(1)
C(2)
25(1)
36(1)
20(1)
−1(1)
9(1)
1(1)
C(3)
24(1)
39(1)
25(1)
−2(1)
11(1)
−3(1)
C(4)
22(1)
43(2)
25(1)
−2(1)
8(1)
−2(1)
C(5)
26(1)
41(1)
20(1)
1(1)
7(1)
2(1)
C(6)
27(1)
46(2)
22(1)
4(1)
8(1)
−6(1)
C(7)
23(1)
43(1)
21(1)
1(1)
8(1)
−2(1)
C(8)
21(1)
39(1)
23(1)
−6(1)
6(1)
−1(1)
C(9)
28(1)
41(2)
28(1)
3(1)
4(1)
−4(1)
C(10)
41(1)
41(2)
30(1)
3(1)
7(1)
−2(1)
C(11)
29(1)
53(2)
28(1)
8(1)
9(1)
−2(1)
C(12)
35(1)
45(2)
24(1)
4(1)
4(1)
−2(1)
C(13)
48(2)
73(2)
29(2)
3(2)
13(1)
10(2)
C(14)
39(2)
39(2)
43(2)
6(1)
20(1)
6(1)
C(15)
43(2)
59(2)
44(2)
18(2)
18(1)
8(2)
C(16)
46(2)
71(2)
61(2)
28(2)
32(2)
17(2)
C(17)
22(1)
43(2)
20(1)
−1(1)
6(1)
−1(1)
C(18)
25(1)
43(2)
21(1)
−3(1)
5(1)
2(1)
C(19)
26(1)
47(2)
24(1)
1(1)
7(1)
5(1)
C(20)
29(1)
44(2)
21(1)
0(1)
5(1)
1(1)
C(21)
26(1)
41(1)
22(1)
1(1)
6(1)
−2(1)
C(22)
33(1)
52(2)
24(1)
−2(1)
7(1)
9(1)
C(23)
46(2)
53(2)
31(1)
−1(1)
8(1)
17(2)
C(24)
27(1)
42(2)
40(2)
−8(1)
11(1)
−8(1)
C(25)
22(2)
31(2)
27(2)
−1(2)
6(2)
−2(2)
C(26)
43(3)
44(3)
33(3)
−3(2)
22(2)
−2(3)
C(27)
35(7)
59(9)
63(8)
18(7)
32(7)
12(6)
C(28)
32(3)
35(3)
37(3)
−4(3)
16(2)
−5(2)
C(29)
30(2)
39(3)
35(3)
4(2)
10(2)
3(2)
C(30)
30(2)
33(3)
23(2)
−1(2)
9(2)
4(2)
C(31)
45(2)
75(3)
57(2)
−23(2)
16(2)
3(2)
C(24A)
27(1)
42(2)
40(2)
−8(1)
11(1)
−8(1)
C(25A)
33(3)
29(3)
34(3)
−4(2)
14(2)
−6(2)
C(26A)
36(5)
45(4)
47(5)
5(4)
13(4)
−15(3)
C(27A)
29(3)
44(3)
49(4)
4(3)
7(3)
−1(3)
C(28A)
25(6)
45(8)
42(7)
5(5)
11(5)
−3(5)
C(29A)
51(3)
42(3)
37(3)
−8(3)
16(3)
−8(3)
C(24X)
27(1)
42(2)
40(2)
−8(1)
11(1)
−8(1)
C(25X)
22(2)
31(2)
27(2)
−1(2)
6(2)
−2(2)
C(26X)
43(3)
44(3)
33(3)
−3(2)
22(2)
−2(3)
C(27X)
44(9)
37(6)
23(6)
−4(6)
13(6)
−5(6)
C(28X)
32(3)
35(3)
37(3)
−4(3)
16(2)
−5(2)
C(29X)
30(2)
39(3)
35(3)
4(2)
10(2)
3(2)
C(30A)
64(4)
37(3)
38(3)
−3(3)
31(3)
−5(3)
C(31A)
45(2)
75(3)
57(2)
−23(2)
16(2)
3(2)
C(32)
46(2)
35(2)
68(2)
13(2)
26(2)
6(1)
C(33)
43(2)
35(2)
49(2)
3(1)
16(1)
6(1)
C(34)
58(2)
62(2)
53(2)
−19(2)
5(2)
20(2)
C(35)
47(2)
55(2)
38(2)
−8(1)
12(1)
12(2)
N(1)
22(1)
51(1)
21(1)
−1(1)
6(1)
−4(1)
N(2)
24(1)
35(1)
26(1)
−1(1)
7(1)
2(1)
N(3)
31(1)
40(1)
24(1)
2(1)
4(1)
−3(1)
N(4)
38(1)
41(1)
30(1)
6(1)
7(1)
−1(1)
N(5)
25(1)
39(1)
22(1)
0(1)
7(1)
0(1)
N(6)
42(1)
44(1)
22(1)
−3(1)
6(1)
3(1)
N(7)
21(5)
43(6)
36(5)
−1(4)
8(4)
−4(4)
N(7A)
34(3)
36(2)
32(2)
−3(2)
12(2)
−6(2)
N(7X)
21(5)
43(6)
36(5)
−1(4)
8(4)
−4(4)
○(1)
50(1)
41(1)
56(1)
4(1)
23(1)
−3(1)
?(2)
23(1)
41(1)
33(1)
−2(1)
4(1)
−2(1)
O(3)
34(2)
33(2)
30(2)
0(2)
5(2)
−1(2)
O(4)
43(2)
41(2)
24(2)
5(2)
4(2)
7(2)
O(3A)
53(2)
39(2)
35(2)
−4(2)
17(2)
−2(2)
O(4A)
97(4)
44(3)
37(2)
−1(2)
18(3)
1(3)
O(5)
71(2)
54(1)
35(1)
2(1)
18(1)
29(1)
O(6)
58(1)
81(2)
35(1)
−7(1)
12(1)
26(1)
F(1)
31(1)
68(1)
29(1)
15(1)
3(1)
−14(1)
F(2)
62(1)
53(1)
43(1)
−18(1)
16(1)
−7(1)
F(3)
38(1)
89(2)
40(1)
−15(1)
13(1)
18(1)
F(4)
67(1)
65(1)
20(1)
0(1)
12(1)
20(1)
Cl(1)
20(1)
58(1)
33(1)
5(1)
7(1)
−1(1)
TABLE 30
Hydrogen coordinates (×104) and isotropic displacement
parameters (Å2 × 103) for Compound A Form C.
x
y
z
U(eq)
H(3)
2094
4900
6159
35
H(9A)
2686
2991
6226
41
H(9B)
2585
2488
6875
41
H(10A)
3003
318
6513
47
H(10B)
3645
1290
6458
47
H(11A)
4627
2163
7459
45
H(11B)
4633
1662
8152
45
H(12)
4301
4321
7896
45
H(13A)
3300
4343
8170
76
H(13B)
3872
3101
8613
76
H(13C)
3172
2535
8006
76
H(15)
4360
34
8631
58
H(16A)
3729
−2904
8391
67
H(16B)
4281
−2230
9105
67
H(20)
667
9873
2817
40
H(23A)
371
12255
3860
69
H(23B)
415
12205
3162
69
H(23C)
1087
12794
3790
69
H(24A)
5159
9612
6800
44
H(24B)
5083
8408
6232
44
H(25)
6334
8724
7401
3
H(26A)
6310
7535
5811
45
H(26B)
7041
6676
6273
45
H(27A)
7151
9561
6150
58
H(27B)
7479
8946
6897
58
H(28A)
6587
10761
6916
41
H(28B)
6031
10253
6197
41
H(29A)
7274
6855
7546
54
H(29B)
6984
5264
7163
54
H(29C)
6601
6002
7597
54
H(31A)
4300
3303
6059
73
H(31B)
4732
2290
5753
73
H(24C)
5704
9215
7028
44
H(24D)
4918
9273
6440
44
H(25A)
5186
6942
5995
38
H(26C)
6557
10107
6574
53
H(26D)
6812
9367
6043
53
H(27C)
7247
7275
6675
52
H(27D)
7066
8103
7237
52
H(28C)
6258
5826
6345
45
H(28D)
6240
6248
7039
45
H(29D)
6112
7305
5353
66
H(29E)
5788
8902
4991
66
H(29F)
5266
7589
5053
66
H(24E)
5159
9612
6800
44
H(24F)
5083
8408
6232
44
H(25X)
6334
8724
7401
33
H(26E)
6551
6676
5911
45
H(26F)
7213
7526
6480
45
H(27E)
6648
9625
5780
42
H(27F)
5858
8986
5653
42
H(28E)
6903
10143
6901
41
H(28F)
6105
10822
6518
41
H(29G)
6606
6030
7603
54
H(29H)
6972
5249
7164
54
H(291)
7280
6841
7539
54
H(31C)
4843
4335
5948
73
H(31D)
4304
3155
6055
73
H(32A)
4255
3655
4793
58
H(32B)
3851
4790
5100
58
H(33A)
3583
1536
5007
52
H(33B)
3112
2832
5159
52
H(34A)
3211
2570
3929
76
H(34B)
2587
1771
4077
76
H(6A)
1386
6164
2951
45
H(6B)
959
7389
2457
45
H(7)
5935
6435
6512
42
H(7A)
5487
9704
5816
41
H(7X)
5935
6435
6512
42
H(5)
2083
5659
4208
82
Similarly to Compound A Form D, the carboxylic group of the adipate forms a heterodimer with the API molecule through the O—H . . . N and O—H . . . N intramolecular interactions. The hydrogen H6A of amine N6 forms one intermolecular N—H . . . O bond to either O3 or O3A oxygen atoms of positionally disordered —COO— group of the adipate anion (50/50). Additionally, the nitrogen atom N7 of one component of positionally disordered 1-methylpyrrolidine is involved in one N—H . . . O intermolecular interaction to oxygen O4 of also disordered —COO— group of adipate. Nitrogen N7A of the second component is hydrogen bonded to the analogous oxygen O4A. There appear to be no further hydrogen bonding interactions and as such the crystal structure packing is further stabilised by Van der Waals interactions only.
Views of the crystal packing within the unit cell can be seen in FIG. 23 and FIG. 24. A comparison of the crystal packing of Compound A Form C and Compound A Form D is shown in FIG. 25. For clarity all hydrogen atoms have been removed from packing diagrams.
Example 6—Compound B Form A
Compound B Form A was obtained from an acetone system and the sample was air dried at RT. No form change was observed before and after drying (FIG. 11). A weight loss of 0.7% up to 100° C. was observed in TGA and DSC result showed one endotherm at 53.8° C. (peak temperature) before the possible overlapped peak with peak temperature at 156.3° C. (FIG. 12). Based on the integrals, the stoichiometric ratio of fumaric acid:freebase was determined to be 1.03. A peak of acetone was observed and approximately 0.49 molar acetone (4.4 wt %) was detected. The HPLC purity of Compound B Form A was determined to be 93.56 area %. After heating Compound B Form A to 100° C. under N2 protection, cooled down and exposed to ambient conditions, no form change was observed before and after heating. Peak of acetone was observed in the heated sample. Around 0.39 molar acetone (3.5 wt %) was still detected. One endotherm at 58.7° C. and an overlapped peak with peak temperature at 157.1° C. were still observed on the sample obtained after heating. The first endotherm might be caused by re-adsorption of moisture. Since ˜3.5 wt % acetone was still detected from NMR, Compound B Form A is expected to be an acetone/H2O co-solvate.
Example 7—Compound C Form A
Compound C Form A was obtained from EtOAc system and the sample was air dried at RT. No form change was observed before and after drying (FIG. 13). A weight loss of 8.6% up to 100° C. was observed in TGA and two endotherms at 81.0° C. and 149.2° C. (peak temperature) were observed in DSC curve (FIG. 14). HPLC purity of Compound C Form A was determined to be 95.18 area %.
Example 8—Compound D Form A
Compound D Form A was obtained from evaporation of acetone/n-heptane (1:1, v/v) solution. The XRPD result is displayed in FIG. 15. A weight loss of 7.7% was observed up to 170° C. in TGA, and DSC result (FIG. 16) showed one endotherm at 75.8° C. (peak temperature). Based on the integrals by NMR analysis, the stoichiometric ratio of benzenesulfonic acid:freebase was determined to be 1.03. Peak of acetone was observed. Around 0.30 molar acetone (2.7 wt %) was detected. HPLC purity of Compound D Form A was determined to be 96.23 area %.
Example 9: Compound E Form A
Compound E Form A was obtained from acetone system. The XRPD spectrum overlay is shown in FIG. 17. Limited solids were observed after stirring at 5° C. During XRPD test, it was observed that the sample tended to absorb moisture and turn to liquid. The suspension was transferred to −20° C., but limited solids were still observed. Anti-solvent (n-heptane) was added and the sample was transferred to 5° C. However, gel was obtained.
Example 10: Compound F Form A
Compound F Form A (810935-03-A2) was obtained from acetone/n-heptane (1:1, v/v) system by evaporation at RT (FIG. 26).
A weight loss of 9.0% up to 100° C. was observed in TGA and DSC result showed two endotherms at 65.5° C. and 125.4° C. (peak temperature) (FIG. 27).
Based on the integrals, the stoichiometric ratio of acetic acid:freebase was determined to be 0.69. Peak of acetone was observed. Around 0.16 molar acetone (1.5 wt %) was detected. The purity of Compound F Form A was 88.42 area %.
After heating Compound F Form A to 100° C. under N2 protection, cooled down and exposed to ambient conditions, no form change was observed. Two broad DSC endotherms at 64.2° C. and 124.2° C. (peak temperature) were still observed on the sample obtained after heating, suggesting the re-adsorption of moisture. Since no form change was observed after heating, Compound F Form A is likely a hydrate.
TABLE 31
Representative XRPD Peaks for Compound F Form A.
Pos. [°2θ]
d-spacing [Å]
Rel. Int. [%]
6.6132
13.35494
55.67
7.7347
11.42087
100
8.9607
9.86079
6.47
10.3787
8.51654
4.48
12.9417
6.83509
21.07
13.7826
6.41992
16.86
14.5599
6.07887
4.79
16.0886
5.50455
12.29
17.4322
5.08318
4.97
18.0779
4.90307
9.75
20.3112
4.36871
20.73
21.2392
4.17987
43.46
24.2764
3.66337
20.25
25.6495
3.47029
8.21
29.6647
3.00907
5.28
Example 10—Freebase Screening Procedure
The solubility of starting material was estimated at RT in 20 solvents. For each experiment, approximately 2 mg of sample was added into a 3-mL glass vial. Solvents in Table 32 were then added stepwise (50, 50, 200, 700 μL) into the vials until the solids were dissolved visually or a total volume of 1 mL was reached. Solubility results are summarized in Table 5-11 and were used to guide the solvent selection in salt screening and crystal form screening.
TABLE 32
Approximate solubility of starting material at RT
Solubility
Solubility
Solvent
(mg/mL)
Solvent
(mg/mL)
MeOH
S > 42.0
1,4-Dioxane
S > 38.0
EtOH
7.0 < S < 21.0
ACN
6.7 < S < 20.0
IPA
2.1 < S < 7.0
MTBE
2.2 < S < 7.3
Acetone
S > 40.0
n-Heptane
S < 2.0
MEK
S > 46.0
Toluene
S > 40.0
EtOAc
S > 40.0
DMSO
S > 38.0
IPAc
S > 40.0
H2O
S < 2.1
MIBK
S > 42.0
DCM
S > 38.0
THF
S > 44.0
CPME
S > 40.0
2-MeTHF
S > 40.0
Anisole
S > 38.0
A total of 64 polymorph screening experiments were performed for freebase Compound 1 using the sample received as starting material through different crystallization methods. The methods utilized and crystal forms identified are summarized in Table 33. As a result, Form A was obtained from polymorph screening.
TABLE 33
Summary of polymorph screening experiments of freebase
Method
Result
Slurry at RT/5 ° C./50 ° C.
Form A, amorphous, gel,
Liquid Vapor Diffusion
Form A, amorphous, gel, clear
Slow Evaporation
Form A, amorphous, gel
Anti-solvent Addition
Form A, amorphous, gel,
Total
Form A, amorphous, gel, clear
Slurry at RT
Slurry conversion experiments were conducted at RT in different solvent systems. About 15˜20 mg of freebase starting material (Compound 1) was suspended in 0.5 mL of solvent in an HPLC vial. Solids were isolated for XRPD analysis after magnetically stirring at RT. Results summarized in Table 34 indicated that Form A and amorphous were obtained.
TABLE 34
Summary of slurry conversion experiments at RT
Solvent, v:v
Result
IPA
Form A (Low crystallinity)
MTBE
Gel
ACN
Form A
EtOH
Form A
EtOH/H2O, 1:1
Form A
ACN/H2O, 1:1
Form A (Low crystallinity)
Acetone/H2O, 1:4
Form A
1,4-Dioxane/H2O, 1:4
Amorphous
Benzyl alcohol/n-Heptane, 1:4
Gel
THF/n-Heptane, 1:4
Form A
DCM/n-Heptane, 1:4
Form A
Anisole/n-Heptane, 1:4
Gel
Toluene/Cyclohexane, 1:4
Amorphous
CPME/Cyclohexane, 1:4
Amorphous
MEK/Cyclohexane, 1:4
Amorphous
EtOAc/Cyclohexane, 1:4
Amorphous
Slurry at 5°. Slurry conversion experiments were conducted at 5° C. in different solvent systems. About 15˜20 mg of freebase starting material (Compound 1) was suspended in 0.5 mL of solvent in an HPLC vial. Solids were isolated for XRPD analysis after magnetically stirring at 5° C. Results summarized in Table 35 indicated that Form A and amorphous were obtained.
TABLE 35
Summary of slurry conversion experiments at 5° C.
Solvent, v:v
Result
ACN
Form A
MIBK/n-Heptane, 1:3
Gel
IPAc/n-Heptane, 1:3
Amorphous
2-MeTHF/n-Heptane, 1:3
Gel
Xylene/n-Heptane, 1:3
Amorphous
DMAc/n-Heptane, 1:3
Gel
NMP/H2O, 1:4
Amorphous
Ethyl lactate/H2O, 1:3
Gel
DMF/H2O, 1:3
Amorphous
Slurry at 50°. Slurry conversion experiments were conducted at 50° C. in different solvent systems. About 20 mg of freebase starting material (Compound 1) was suspended in 0.5 mL of solvent in an HPLC vial. Solids were isolated for XRPD analysis after magnetical stirring at 50° C. Results summarized in Table 36 indicated that amorphous was obtained.
TABLE 36
Solvent
Result
H2O
Amorphous
n-Heptane
Amorphous
Liquid vapor diffusion. Liquid vapor diffusion experiments were conducted in different solvent systems. Approximate 20 mg of freebase starting material (Compound 1) was dissolved in 0.3˜1.5 mL corresponding solvent to obtain a clear solution in a 3-mL vial (if a suspension was observed, the sample was filtered through a PTFE filter with 0.45 μm pore size). This solution was then placed into a 20-mL vial with 3 mL of corresponding anti-solvent. The 20-mL vial was sealed with a cap and kept at RT allowing sufficient time for organic vapor to interact with the solution. The precipitates were isolated for XRPD analysis. The results summarized in Table 37 showed that Form A and amorphous were observed.
TABLE 37
Solvent
Anti-solvent
Result
IPAc
n-Heptane
Amorphous
Toluene
Gel
1.4-Dioxane
Gel
2-Butanol
Gel
DMF
H2O
Clear solution
ACN
Form A
DMSO
Amorphous
THF
Form A (Low crystallinity)
CPME
n-Pentane
Gel
Anisole
Gel
Acetone
Form A
EtOAc
Gel
Xylene
Gel
Slow evaporation. Slow evaporation experiments were performed under 10 conditions. Briefly, about 15˜20 mg of freebase starting material (810935-01-A) was dissolved in 0.5˜1.0 mL of solvent in a 3-mL glass vial. The visually clear solutions were subjected to evaporation at RT with vials sealed by Parafilm®. The solids were isolated for XRPD analysis, and the results summarized in Table 38 indicated that Form A and amorphous were obtained.
TABLE 38
Solvent
Result
ACN
Form A
DCM
Form A (Low crystallinity)
MEK
Amorphous
EtOAc
Amorphous
IPAc
Gel
MeOH
Amorphous
EtOH
Form A
Acetone
Form A
THF
Amorphous
2-MeTHF
Gel
Anti-solvent addition. A total of 12 anti-solvent addition experiments were carried out. About 20 mg of freebase starting material (Compound 1) was dissolved in 0.5˜1.5 mL solvent to obtain a clear solution (if a suspension was observed, the sample was filtered through a PTFE filter with 0.45 μm pore size), and the solution was magnetically stirred followed by addition of anti-solvent stepwise till precipitate appeared or the total amount of anti-solvent reached 10.0 mL. The obtained precipitate was isolated for XRPD analysis. Results summarized in Table 39 showed that Compound A Form A with low crystallinity and amorphous were generated.
TABLE 39
Solvent
Anti-solvent
Result
Toluene
n-Heptane
Amorphous
EtOAc
Amorphous
CPME
Amorphous
Acetone
Form A (Low
crystallinity)
ACN
Form A (Low
crystallinity)
1.4-Dioxane
H2O
Gel
MeOH
Amorphous
DMSO
Low crystallinity
THF
Form A (Low
crystallinity)
Anisole
Cyclohexane
Gel
MEK
Gel
DCM
Form A (Low
crystallinity)
Example 11—Polymorphic Screening of Compound A
The solubility of Compound A Form A (810935-33-A) was estimated at RT, following similar procedure as described herein. Results summarized in Table 40 were used to guide the solvent selection in polymorph screening of adipate. The methods utilized and crystal forms identified are summarized in Table 41.
TABLE 40
Approximate solubility of Compound A Form A at RT
Solvent
Solubility (mg/mL)
Solvent
Solubility (mg/mL)
MeOH
S > 48.0
1,4-Dioxane
7.0 < S < 21.0
EtOH
S > 42.0
ACN
2.4 < S < 8.0
IPA
2.2 < S < 7.3
MTBE
S < 1.9
Acetone
6.0 < S < 18.0
n-Heptane
S < 2.0
MEK
6.7 < S < 20.0
Toluene
S < 1.9
EtOAc
S < 2.0
DMSO
S > 44.0
IPAc
S < 1.9
H2O
22.0 < S < 44.0
MIBK
S < 2.0
DCM
19.0 < S < 38.0
THF
S > 48.0
CPME
S < 2.0
2-MeTHF
20.0 < S < 40.0
Anisole
S < 1.9
TABLE 41
Summary of polymorph screening experiments of adipate
Method
Result
Slurry at RT/50° C.
Compound A Form A, gel, clear
Liquid Vapor Diffusion
Amorphous, clear, gel
Slow Evaporation
Gel, clear
Solid Vapor Diffusion
Compound A Form A
Anti-solvent Addition
Compound A Form A, B, clear, gel
Slow Cooling
Compound A Form A
Total
Compound A Form A, Compound A Form
B, clear, gel
Slurry at RT for Compound A. Slurry conversion experiments were conducted at RT in different solvent systems. About 15 mg of Compound A Form A was suspended in 0.5 mL of solvent in an HPLC vial. Solids were isolated for XRPD analysis after magnetic stirring at RT. Results summarized in Table 42 indicated that adipate Type A was obtained.
TABLE 42
Solvent, v:v
Result
IPA
Compound A Form A
ACN
Compound A Form A
Acetone
Compound A Form A
MEK
Compound A Form A
1,4-Dioxane
Compound A Form A
H2O
Clear solution
H2O/ACN, 1:4
Gel
H2O/IPA, 1:4
Gel
DCM/IPA, 1:4
Compound A Form A
2-MeTHF/Toluene, 1:4
Compound A Form A
Acetone/n-Heptane, 1:3
Compound A Form A
Acetone/Anisole, 1:3
Compound A Form A
MEK/n-Heptane, 1:3
Compound A Form A
MEK/MTBE, 1:3
Compound A Form A
1,4-Dioxane/n-Heptane, 1:3
Compound A Form A
1,4-Dioxane/IPAc, 1:3
Compound A Form A
DMSO/H2O, 1:6
Clear solution
THF/H2O, 1:6
Clear solution
EtOH/n-Heptane, 1:6
Compound A Form A
MeOH/CPME, 1:6
Compound A Form A
*: Clear solution was transferred to 5° C., followed by transferring to −20° C.
**: Clear solution was transferred to 5° C., followed by transferring to −20° C. Clear solution was still observed, so anti-solvent was added.
#: Clear solution was transferred to 5° C., followed by transferring to −20° C. Clear solution was still observed, so anti-solvent was added. Since clear solution was still observed, the sample was transferred to evaporation at RT.
&: The clear solution was transferred to evaporation at RT
Slurry at 50° for Compound A. Slurry conversion experiments were conducted at 50° C. in different solvent systems. About 15 mg of Compound A Form A was suspended in 0.5 mL of solvent in an HPLC vial. Solids were isolated for XRPD analysis after magnetic stirring at 50° C. Results summarized in Table 43 indicated that Compound A Form A was obtained.
TABLE 43
Solvent
Result
MIBK
Compound A Form A
EtOAc
Compound A Form A
IPAc
Compound A Form A
Anisole
Compound A Form A
n-Heptane
Compound A Form A
CPME
Compound A Form A
MTBE
Compound A Form A
Toluene
Compound A Form A
Liquid vapor diffusion Compound A. Liquid vapor diffusion experiments were conducted in different solvent systems. Approximate 15 mg of Compound A Form A was dissolved in 0.5 mL corresponding solvent to obtain a clear solution in a 3-mL vial. This solution was then placed into a 20-mL vial with 3 mL of corresponding anti-solvent. The 20-mL vial was sealed with a cap and kept at RT allowing sufficient time for organic vapor to interact with the solution. The precipitates were isolated for XRPD analysis. The results summarized in Table 44 showed that amorphous was obtained.
TABLE 44
Solvent
Anti-solvent
Result
DMSO
EtOAc
Clear solution
THF
n-Heptane
Amorphous
MTBE
Gel
EtOH
n-Pentane
Gel
MTBE
Gel
H2O
IPA
Gel
ACN
Gel
*: clear solutions obtained from liquid vapor diffusion were transferred to evaporation at RT.
Slow evaporation Compound A. Slow evaporation experiments were performed under seven conditions. Briefly, about 15 mg of Compound A Form A was dissolved in 0.5˜1.0 mL of solvent in a 3-mL glass vial. The visually clear solutions were subjected to evaporation at RT with vials sealed by Parafilm® with a few pinholes. The results summarized in Table 45 indicated that only gel or clear solution was obtained.
TABLE 45
Solvent
Result
MeOH
Gel
EtOH
Gel
THF
Gel
DCM
Gel
2-MeTHF
Gel
H2O
Clear solution
Acetone
Gel
Solid vapor diffusion Compound A. Solid vapor diffusion experiments were conducted using 12 different solvents. Approximate 15 mg of Compound A Form A (810935-40-A) was weighed into a 3-mL vial, which was placed into a 20-mL vial with 2 mL of corresponding solvent. The 20-mL vial was sealed with a cap and kept at RT allowing solvent vapor to interact with the sample. The solids were tested by XRPD and the results summarized in Table 46 showed that Compound A Form A was obtained.
TABLE 46
Solvent
Result
H2O
Compound A Form A
DCM
Compound A Form A
EtOH
Compound A Form A
MeOH
Compound A Form A
ACN
Compound A Form A
THF
Compound A Form A
Acetone
Compound A Form A
DMF
Compound A Form A
EtOAc
Compound A Form A
1,4-Dioxane
Compound A Form A
IPA
Compound A Form A
DMSO
Compound A Form A
Anti-solvent addition Compound A. A total of 14 anti-solvent addition experiments were carried out. About 15 mg of Compound A Form A was dissolved in 0.5˜1.5 mL solvent to obtain a clear solution (if a suspension was observed, the sample was filtered through a PTFE filter with 0.45 μm pore size), and the solution was magnetically stirred followed by addition of anti-solvent stepwise until precipitate appeared or the total amount of anti-solvent reached 10.0 mL. The obtained precipitate was isolated for XRPD analysis. Results summarized in Table 47 showed that Compound A Form A and Compound A Form B were generated.
TABLE 47
Solvent
Anti-solvent
Result
THF
n-Heptane
Compound A Form A
EtOH
Compound A Form A
DCM
Compound A Form A
2-MeTHF
Gel
EtOH
Anisole
Clear solution
DMSO
EtOAc
Clear
THF
Compound A Form A
MeOH
Toluene
Compound A Form A
THF
Compound A Form A
DCM
Compound A Form B
MeOH
MTBE
Gel
EtOH
Gel
DCM
Compound A Form A
THF
Compound A Form A
Slow cooling Compound A. Slow cooling experiments were conducted in four solvent systems. About 15 mg of Compound A Form A was suspended in 1.0 mL of solvent in a 3-mL glass vial at RT. The suspension was then heated to 50° C., equilibrated for about 2 hr and filtered to a new vial using a seal membrane (PTFE, pore size of 0.45 μm). Filtrates were slowly cooled down to 5° C. at a rate of 0.1° C./min. The obtained solids were kept isothermal at 5° C. before isolation for XRPD analysis. Results summarized in Table 48 indicated Compound A Form A was obtained.
TABLE 48
Solvent
Result
Acetone
Compound A Form A
MEK
Compound A Form A
IPA
Compound A Form A
ACN
Compound A Form A
All technical and scientific terms used herein have the same meaning. Efforts have been made to ensure accuracy with respect to numbers used (e.g. amounts, temperature, etc.) but some experimental errors and deviations should be accounted for.
Throughout this specification and the claims, the words “comprise,” “comprises,” and “comprising” are used in a non-exclusive sense, except where the context requires otherwise. It is understood that embodiments described herein include “consisting of” and/or “consisting essentially of” embodiments.
Where a range of values is provided, it is understood that each intervening value, to the tenth of the unit of the lower limit, unless the context clearly dictates otherwise, between the upper and lower limit of the range and any other stated or intervening value in that stated range, is encompassed herein. The upper and lower limits of these small ranges which can independently be included in the smaller rangers is also encompassed herein, subject to any specifically excluded limit in the stated range. Where the stated range includes one or both of the limits, ranges excluding either or both of those included limits are also included herein.
Many modifications and other embodiments of the inventions set forth herein will come to mind to one skilled in the art to which these inventions pertain having the benefit of the teachings presented in the foregoing descriptions and the associated drawings. Therefore, it is to be understood that the inventions are not to be limited to the specific embodiments disclosed and that modifications and other embodiments are intended to be included within the scope of the appended claims. Although specific terms are employed herein, they are used in a generic and descriptive sense only and not for purposes of limitation.Inventors (1)
- Antonio Giovanni DipasqualeSan Bruno, CA, US
Assignees (1)
- Genentech, Inc.South San Francisco, CA, US
CPC (3)
C07D401/14A61P35/00C07B2200/13
IPC (2)
A61P35/00C07D401/14
Backward citations (7)
US11236068[B2]US2022/0081413[A1]US2023/0089126[A1]WOWO-2020097537[A2]WO2022/035790[A1]WO2022/103904[A1]WO2022/125427[A1]
Source: ipg260303.zip (2026-03-03)